Your search keyword '"Complement C3b metabolism"' showing total 114 results

1. Three Years On: The Role of Pegcetacoplan in Paroxysmal Nocturnal Hemoglobinuria (PNH) since Its Initial Approval.

Author

Horneff R, Czech B, Yeh M, and Surova E

Subjects

Humans, Hemolysis drug effects, Complement Inactivating Agents therapeutic use, Complement C3b metabolism, United States Food and Drug Administration, Hemoglobinuria, Paroxysmal drug therapy, Antibodies, Monoclonal, Humanized therapeutic use, Drug Approval, Complement C3 metabolism

Abstract

Paroxysmal nocturnal hemoglobinuria (PNH) is a rare disease characterized by complement-mediated hemolysis and potentially life-threatening complications. Pegcetacoplan, an inhibitor of complement components C3 and C3b, was approved by the US Food and Drug Administration (FDA) and European Medicines Agency (EMA) in 2021. A recent expansion to its indication by the EMA has made pegcetacoplan available for the treatment of both complement inhibitor-naïve and -experienced patients with PNH who have hemolytic anemia, a similarly broad patient population as in the US. This approval was based on results from the Phase 3 PEGASUS study, where pegcetacoplan showed superiority over the C5 inhibitor eculizumab with regard to improving the hemoglobin level in patients with anemia despite eculizumab treatment, and the Phase 3 PRINCE study, where pegcetacoplan showed superiority over supportive care with regard to hemoglobin stabilization and improving the lactate dehydrogenase level in complement inhibitor-naïve patients. In light of this recent indication expansion by the EMA, this article describes how the strong efficacy of pegcetacoplan is linked to its mechanism of action, which provides broad hemolysis control over both intravascular and extravascular hemolysis to improve a range of disease markers and enhance patients' quality of life. Furthermore, additional data and learnings obtained from over 3 years of experience with pegcetacoplan are summarized, including long-term efficacy and safety results, real-world clinical experiences, pharmacokinetic characteristics, and extensive practical guidance for the first-to-market proximal complement inhibitor for PNH.

Published

2024

2. C3-dependent effector functions of complement.

Author

Zarantonello A, Revel M, Grunenwald A, and Roumenina LT

Subjects

Humans, Receptors, Complement analysis, Binding Sites, Complement Activation, Complement C3 analysis, Complement C3 metabolism, Complement C3b metabolism

Abstract

C3 is the central effector molecule of the complement system, mediating its multiple functions through different binding sites and their corresponding receptors. We will introduce the C3 forms (native C3, C3 [H 2 O], and intracellular C3), the C3 fragments C3a, C3b, iC3b, and C3dg/C3d, and the C3 expression sites. To highlight the important role that C3 plays in human biological processes, we will give an overview of the diseases linked to C3 deficiency and to uncontrolled C3 activation. Next, we will present a structural description of C3 activation and of the C3 fragments generated by complement regulation. We will proceed by describing the C3a interaction with the anaphylatoxin receptor, followed by the interactions of opsonins (C3b, iC3b, and C3dg/C3d) with complement receptors, divided into two groups: receptors bearing complement regulatory functions and the effector receptors without complement regulatory activity. We outline the molecular architecture of the receptors, their binding sites on the C3 activation fragments, the cells expressing them, the diversity of their functions, and recent advances. With this review, we aim to give an up-to-date analysis of the processes triggered by C3 activation fragments on different cell types in health and disease contexts., (© 2022 The Authors. Immunological Reviews published by John Wiley & Sons Ltd.)

Published

2023

3. Initiation of the alternative pathway of complement and the history of "tickover".

Author

Pangburn MK

Subjects

Humans, Complement Activation, Antibodies, Sulfur Compounds, Complement Pathway, Alternative, Complement C3 metabolism, Complement C3b metabolism

Abstract

The evolutionary history of complement suggests that the alternative pathway arose prior to the arrival of the classical and lectin pathways. In these pathways, target specificity is provided by antibodies and sugar specific lectins. While these efficient initiation systems dominate activation on most targets, the alternative pathway produces most of the C3b and 80%-90% of the C5b-9. While the tickover process, originally proposed by Peter Lachmann, provided ancient hosts with a crude self/non-self-discriminatory system that initiated complement attack on everything foreign, tickover clearly plays a more minor role in complement activation in modern organisms possessing classical and lectin pathways. Spontaneous activation of the alternative pathway via tickover may play a major role in human pathologies where tissue damage is complement-mediated. The molecular mechanism of tickover is still not convincingly proven. Prevailing hypotheses include (a) spontaneous hydrolysis of the thioester in C3 forming the C3b-like C3(H 2 O) in solution and (b) "enhanced tickover" in which surfaces cause specific or non-specific contact activated conformational changes in C3. Theoretical considerations, including computer simulations, suggest that the latter mechanism is more likely and that more research needs to be devoted to understanding interactions between biological surfaces and C3., (© 2022 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2023

4. Structure-Guided Engineering of a Complement Component C3-Binding Nanobody Improves Specificity and Adds Cofactor Activity.

Author

Pedersen H, Jensen RK, Hansen AG, Petersen SV, Thiel S, Laursen NS, and Andersen GR

Subjects

Animals, Complement Activation, Complement C3 Convertase, Alternative Pathway, Complement C3-C5 Convertases metabolism, Fibrinogen metabolism, Humans, Rats, Complement C3, Complement C3b metabolism

Abstract

The complement system is a part of the innate immune system, where it labels intruding pathogens as well as dying host cells for clearance. If complement regulation is compromised, the system may contribute to pathogenesis. The proteolytic fragment C3b of complement component C3, is the pivot point of the complement system and provides a scaffold for the assembly of the alternative pathway C3 convertase that greatly amplifies the initial complement activation. This makes C3b an attractive therapeutic target. We previously described a nanobody, hC3Nb1 binding to C3 and its degradation products. Here we show, that extending the N-terminus of hC3Nb1 by a Glu-Trp-Glu motif renders the resulting EWE-hC3Nb1 (EWE) nanobody specific for C3 degradation products. By fusing EWE to N-terminal CCP domains from complement Factor H (FH), we generated the fusion proteins EWEnH and EWEµH. In contrast to EWE, these fusion proteins supported Factor I (FI)-mediated cleavage of human and rat C3b. The EWE, EWEµH, and EWEnH proteins bound C3b and iC3b with low nanomolar dissociation constants and exerted strong inhibition of alternative pathway-mediated deposition of complement. Interestingly, EWEnH remained soluble above 20 mg/mL. Combined with the observed reactivity with both human and rat C3b as well as the ability to support FI-mediated cleavage of C3b, this features EWEnH as a promising candidate for in vivo studies in rodent models of complement driven pathogenesis., Competing Interests: Authors HP, RJ, NL, ST and GA are listed as inventors on a patent describing the use of EWE, hC3Nb2 and hC3Nb3. Authors HP, RJ, NL and GA have filed the patent application P6053EP00 for the use of EWEµH and EWEnH. 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 © 2022 Pedersen, Jensen, Hansen, Petersen, Thiel, Laursen and Andersen.)

Published

2022

5. Complement component C3: A structural perspective and potential therapeutic implications.

Author

Geisbrecht BV, Lambris JD, and Gros P

Subjects

Humans, Complement Activation, Complement C3b chemistry, Complement C3b metabolism, Complement C3 metabolism

Abstract

As the most abundant component of the complement system, C3 and its proteolytic derivatives serve essential roles in the function of all three complement pathways. Central to this is a network of protein-protein interactions made possible by the sequential proteolysis and far-reaching structural changes that accompany C3 activation. Beginning with the crystal structures of C3, C3b, and C3c nearly twenty years ago, the physical transformations underlying C3 function that had long been suspected were finally revealed. In the years that followed, a compendium of crystallographic information on C3 derivatives bound to various enzymes, regulators, receptors, and inhibitors generated new levels of insight into the structure and function of the C3 molecule. This Review provides a concise classification, summary, and interpretation of the more than 50 unique crystal structure determinations for human C3. It also highlights other salient features of C3 structure that were made possible through solution-based methods, including Hydrogen/Deuterium Exchange and Small Angle X-ray Scattering. At this pivotal time when the first C3-targeted therapeutics begin to see use in the clinic, some perspectives are also offered on how this continually growing body of structural information might be leveraged for future development of next-generation C3 inhibitors., (Copyright © 2022 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published

2022

6. von Willebrand factor variants in C3 glomerulopathy: A Chinese cohort study.

Author

Chen YY, Han SS, Cao Y, Yu XJ, Zhu L, Luo JC, Song WC, Yu F, Mao YH, and Zhao MH

Subjects

Adolescent, Adult, Case-Control Studies, China, Cohort Studies, Complement C3b metabolism, Complement Factor H metabolism, Complement Pathway, Alternative, Female, Genetic Variation, Glomerulonephritis immunology, Glomerulonephritis pathology, Glomerulonephritis, Membranoproliferative immunology, Glomerulonephritis, Membranoproliferative pathology, High-Throughput Nucleotide Sequencing, Humans, In Vitro Techniques, Kidney Glomerulus immunology, Kidney Glomerulus pathology, Male, Middle Aged, Models, Immunological, Molecular Dynamics Simulation, Recombinant Proteins chemistry, Recombinant Proteins genetics, Recombinant Proteins metabolism, Sequence Analysis, DNA, Young Adult, von Willebrand Factor chemistry, von Willebrand Factor metabolism, Complement C3 metabolism, Glomerulonephritis genetics, Glomerulonephritis, Membranoproliferative genetics, von Willebrand Factor genetics

Abstract

C3 glomerulopathy (C3G) is a rare renal disease characterized by predominant glomerular C3 staining. Complement alternative pathway dysregulation due to inherited complement defects is associated with C3G. To identify novel C3G-related genes, we screened 86 genes in the complement, coagulation and endothelial systems in 35 C3G patients by targeted genomic enrichment and massively parallel sequencing. Surprisingly, the most frequently mutated gene was VWF. Patients with VWF variants had significantly higher proteinuria levels, higher crescent formation and lower factor H (FH) levels. We further selected two VWF variants to transiently express the von Willebrand factor (vWF) protein, we found that vWF expression from the c.1519A > G variant was significantly reduced. In vitro results further indicated that vWF could regulate complement activation, as it could bind to FH and C3b, act as a cofactor for factor I-mediated cleavage of C3b. Thus, we speculated that vWF might be involved in the pathogenesis of C3G., (Copyright © 2021 Elsevier Inc. All rights reserved.)

Published

2021

7. Characterization of Binding Properties of Individual Functional Sites of Human Complement Factor H.

Author

Haque A, Cortes C, Alam MN, Sreedhar M, Ferreira VP, and Pangburn MK

Subjects

Binding Sites, Complement C3 immunology, Complement C3b metabolism, Complement C3d metabolism, Complement Factor H genetics, Complement Factor H immunology, Complement Factor H metabolism, Complement Pathway, Alternative, Humans, Immunity, Innate, Kinetics, Ligands, Protein Binding, Protein Interaction Domains and Motifs, Recombinant Proteins metabolism, Structure-Activity Relationship, Complement C3 metabolism

Abstract

Factor H exists as a 155,000 dalton, extended protein composed of twenty small domains which is flexible enough that it folds back on itself. Factor H regulates complement activation through its interactions with C3b and polyanions. Three binding sites for C3b and multiple polyanion binding sites have been identified on Factor H. In intact Factor H these sites appear to act synergistically making their individual contributions difficult to distinguish. Recombinantly expressed fragments of human Factor H were examined using surface plasmon resonance (SPR) for interactions with C3, C3b, iC3b, C3c, and C3d. Eleven recombinant proteins of lengths from one to twenty domains were used to show that the three C3b-binding sites exhibit 100-fold different affinities for C3b. The N-terminal site [complement control protein (CCP) domains 1-6] bound C3b with a K d of 0.08 μM and this interaction was not influenced by the presence or absence of domains 7 and 8. Full length Factor H similarly exhibited a K d for C3b of 0.1 μM. Unexpectedly, the N-terminal site (CCP 1-6) bound native C3 with a K d of 0.4 μM. The C-terminal domains (CCP 19-20) exhibited a K d of 1.7 μM for C3b. We localized a weak third C3b binding site in the CCP 13-15 region with a K d estimated to be ~15 μM. The C-terminal site (CCP 19-20) bound C3b, iC3b, and C3d equally well with a K d of 1 to 2 μM. In order to identify and compare regions of Factor H that interact with polyanions a family of 18 overlapping three domain recombinant proteins spanning the entire length of Factor H were expressed and purified. Immobilized heparin was used as a model polyanion and SPR confirmed the presence of heparin binding sites in CCP 6-8 ( K d 1.2 μM) and in CCP 19-20 (4.9 μM) and suggested the existence of a weak third polyanion binding site in the center of Factor H (CCP 11-13). Our results unveil the relative contributions of different regions of Factor H to its regulation of complement, and may contribute to the understanding of how defects in certain Factor H domains lead to disease., (Copyright © 2020 Haque, Cortes, Alam, Sreedhar, Ferreira and Pangburn.)

Published

2020

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. Complement C3 opsonization of Chlamydia trachomatis facilitates uptake in human monocytes.

Author

Lausen M, Christiansen G, Karred N, Winther R, Poulsen TBG, Palarasah Y, and Birkelund S

Subjects

Cells, Cultured, Complement C3b metabolism, Cytokines metabolism, Microbial Viability, Monocytes metabolism, Monocytes microbiology, Phagocytosis, Serogroup, Chlamydia Infections immunology, Chlamydia trachomatis immunology, Complement C3 metabolism, Host-Pathogen Interactions immunology, Monocytes immunology, Opsonin Proteins metabolism

Abstract

Chlamydia trachomatis is an obligate intracellular bacterium that causes severe infections, which can lead to infertility and ectopic pregnancy. Although both innate and adaptive immune responses are elicited during chlamydial infection the bacterium succeeds to evade host defense mechanisms establishing chronic infections. Thus, studying the host-pathogen interaction during chlamydial infection is of importance to understand how C. trachomatis can cause chronic infections. Both the complement system and monocytes play essential roles in anti-bacterial defense, and, therefore, we investigated the interaction between the complement system and the human pathogens C. trachomatis D and L2. Complement competent serum facilitated rapid uptake of both chlamydial serovars into monocytes. Using immunoelectron microscopy, we showed that products of complement C3 were loosely deposited on the bacterial surface in complement competent serum and further characterization demonstrated that the deposited C3 product was the opsonin iC3b. Using C3-depleted serum we confirmed that complement C3 facilitates rapid uptake of chlamydiae into monocytes in complement competent serum. Complement facilitated uptake did not influence intracellular survival of C. trachomatis or C. trachomatis-induced cytokine secretion. Hence, C. trachomatis D and L2 activate the complement system leading to chlamydial opsonization by iC3b and subsequent phagocytosis, activation and bacterial elimination by human monocytes., (Copyright © 2018 Institut Pasteur. Published by Elsevier Masson SAS. All rights reserved.)

Published

2018

10. An Engineered Complement Factor H Construct for Treatment of C3 Glomerulopathy.

Author

Yang Y, Denton H, Davies OR, Smith-Jackson K, Kerr H, Herbert AP, Barlow PN, Pickering MC, and Marchbank KJ

Subjects

Animals, Complement Factor H chemical synthesis, Complement Factor H genetics, Complement Pathway, Alternative, Cricetinae, Glomerular Basement Membrane metabolism, Glomerulonephritis, Membranoproliferative drug therapy, Half-Life, Mice, Protein Binding, Protein Engineering, Complement C3 metabolism, Complement C3b metabolism, Complement Factor H metabolism, Complement Factor H pharmacokinetics, Glomerulonephritis, Membranoproliferative metabolism

Abstract

Background C3 glomerulopathy (C3G) is associated with dysregulation of the alternative pathway of complement activation, and treatment options for C3G remain limited. Complement factor H (FH) is a potent regulator of the alternative pathway and might offer a solution, but the mass and complexity of FH makes generation of full-length FH far from trivial. We previously generated a mini-FH construct, with FH short consensus repeats 1-5 linked to repeats 18-20 (FH 1-5^18-20 ), that was effective in experimental C3G. However, the serum t 1/2 of FH 1-5^18-20 was significantly shorter than that of serum-purified FH. Methods We introduced the oligomerization domain of human FH-related protein 1 (denoted by R1-2) at the carboxy or amino terminus of human FH 1-5^18-20 to generate two homodimeric mini-FH constructs (FH R1-2^1-5^18-20 and FH 1-5^18-20^R1-2 , respectively) in Chinese hamster ovary cells and tested these constructs using binding, fluid-phase, and erythrocyte lysis assays, followed by experiments in FH-deficient Cfh-/- mice. Results FH R1-2^1-5^18-20 and FH 1-5^18-20^R1-2 homodimerized in solution and displayed avid binding profiles on clustered C3b surfaces, particularly FH R1-2^1-5^18-20 Each construct was >10-fold more effective than FH at inhibiting cell surface complement activity in vitro and restricted glomerular basement membrane C3 deposition in vivo significantly better than FH or FH 1-5^18-20 FH 1-5^18-20^R1-2 had a C3 breakdown fragment binding profile similar to that of FH, a >5-fold increase in serum t 1/2 compared with that of FH 1-5^18-20 , and significantly better retention in the kidney than FH or FH 1-5^18-20 Conclusions FH 1-5^18-20^R1-2 may have utility as a treatment option for C3G or other complement-mediated diseases., (Copyright © 2018 by the American Society of Nephrology.)

Published

2018

11. Experimental confirmation of the C3 tickover hypothesis by studies with an Ab (S77) that inhibits tickover in whole serum.

Author

Lachmann PJ, Lay E, and Seilly DJ

Subjects

Animals, Antibody Specificity, Complement C3b metabolism, Complement Factor B metabolism, Complement Pathway, Alternative immunology, Complement Pathway, Classical, Fibrinogen metabolism, Humans, Immunoglobulin G metabolism, Peptide Library, Rabbits, Complement C3 metabolism, Models, Immunological

Abstract

The complement component 3 (C3) tickover hypothesis was put forward in the early 1970s to account for the spontaneous activation of the alternative complement pathway that occurs after the genetic absence or in vitro depletion of Factor I, the enzyme that is essential for the breakdown of C3b. The hypothesis was widely accepted, but experimental demonstration of the tickover was elusive. A phage Ab against C3b that inhibited the alternative complement pathway, but not the classical pathway, was described in 2009. Studies using this Ab in a variety of assays have now demonstrated that it acts primarily by inhibiting tickover, thereby confirming that tickover really exists.-Lachmann, P. J., Lay, E., Seilly, D. J. Experimental confirmation of the C3 tickover hypothesis by studies with an Ab (S77) that inhibits tickover in whole serum., (© FASEB.)

Published

2018

12. 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

13. Characterization of C3 in C3 glomerulopathy.

Author

Sethi S, Vrana JA, Fervenza FC, Theis JD, Sethi A, Kurtin PJ, Zhang Y, and Smith RJH

Subjects

Adolescent, Adult, Amino Acid Sequence, Biopsy, Child, Chromatography, Liquid, Complement C3a metabolism, Complement C3b metabolism, Female, Glomerulonephritis pathology, Glomerulonephritis, Membranoproliferative pathology, Humans, Kidney Glomerulus ultrastructure, Male, Mass Spectrometry, Microscopy, Electron, Microscopy, Fluorescence, Middle Aged, Peptide Fragments metabolism, Young Adult, Complement C3 metabolism, Glomerulonephritis metabolism, Glomerulonephritis, Membranoproliferative metabolism, Kidney Glomerulus metabolism

Abstract

Background: C3 glomerulopathy (C3G) is caused by overactivity of the alternative pathway of complement that results in bright glomerular C3 staining with minimal or no deposition of immunoglobulins on immunofluorescence microscopy. Laser microdissection and mass spectrometry of the two subtypes, C3 glomerulonephritis (C3GN) and dense deposit disease (DDD), have identified C3 as the predominant glomerular complement protein, although lesser amounts of C9, C5, C6, C7 and C8 are detectable. C3 plays a central role in complement activity, with its proteolytic cleavage first generating C3a and C3b, followed by inactivation of C3b generating iC3b (which includes C3α and C3β), which undergoes further breakdown yielding C3c and terminal breakdown fragment C3dg. The composition of C3 breakdown products in C3G is not known., Methods: In this study, we chose six cases each of C3GN and DDD to analyze the composition of C3 deposits. We analyzed the amino acid sequence of C3 spectra detected by mass spectrometry to determine the relative abundance of C3 fragments in C3G. Thus we were able to determine the amino acid sequences mapping to the various C3 activation products including C3dg, C3α (C3α1 and α2), and C3β that are part of C3b/iC3b/C3c., Results: C3dg is the predominant cleavage product detected with the highest amino acid coverage. The remaining amino acids map to C3α (C3α1 and α2) and C3β. Amino acids mapping to C3a and C3f are absent. Taken together, the C3α and C3β amino acids represent iC3b prior to or after C3c cleavage of C3dg. The C3 spectra for both C3GN and DDD are surprisingly similar., Conclusion: The finding of large amounts of C3dg suggests that C3b deposition in the glomerulus is an active process triggered by thioester binding of C3b to the glycocalyx overlying the glomerular endothelial cells and glomerular basement membrane. Regulatory protein-mediated inactivation of C3b results in the generation of iC3b. After additional cleavages, mostly C3dg remains., (© The Author 2016. Published by Oxford University Press on behalf of ERA-EDTA. All rights reserved.)

Published

2017

14. 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

15. 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

16. 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

17. A rare nonsynonymous sequence variant in C3 is associated with high risk of age-related macular degeneration.

Author

Helgason H, Sulem P, Duvvari MR, Luo H, Thorleifsson G, Stefansson H, Jonsdottir I, Masson G, Gudbjartsson DF, Walters GB, Magnusson OT, Kong A, Rafnar T, Kiemeney LA, Schoenmaker-Koller FE, Zhao L, Boon CJ, Song Y, Fauser S, Pei M, Ristau T, Patel S, Liakopoulos S, van de Ven JP, Hoyng CB, Ferreyra H, Duan Y, Bernstein PS, Geirsdottir A, Helgadottir G, Stefansson E, den Hollander AI, Zhang K, Jonasson F, Sigurdsson H, Thorsteinsdottir U, and Stefansson K

Subjects

Amino Acid Substitution, Base Sequence, Complement Activation genetics, Complement C3b immunology, Complement Factor H immunology, Complement Factor H metabolism, Gene Frequency, Genetic Predisposition to Disease, Genetic Variation, Genome-Wide Association Study, Genotype, Humans, Iceland, Polymorphism, Single Nucleotide, Risk, Sequence Analysis, DNA, Complement C3 genetics, Complement C3b metabolism, Macular Degeneration genetics

Abstract

Through whole-genome sequencing of 2,230 Icelanders, we detected a rare nonsynonymous SNP (minor allele frequency = 0.55%) in the C3 gene encoding a p.Lys155Gln substitution in complement factor 3, which, following imputation into a set of Icelandic cases with age-related macular degeneration (AMD) and controls, associated with disease (odds ratio (OR) = 3.45; P = 1.1 × 10(-7)). This signal is independent of the previously reported common SNPs in C3 encoding p.Pro314Leu and p.Arg102Gly that associate with AMD. The association of p.Lys155Gln was replicated in AMD case-control samples of European ancestry with OR = 4.22 and P = 1.6 × 10(-10), resulting in OR = 3.65 and P = 8.8 × 10(-16) for all studies combined. In vitro studies have suggested that the p.Lys155Gln substitution reduces C3b binding to complement factor H, potentially creating resistance to inhibition by this factor. This resistance to inhibition in turn is predicted to result in enhanced complement activation.

Published

2013

18. Streptococcus pneumoniae capsular serotype invasiveness correlates with the degree of factor H binding and opsonization with C3b/iC3b.

Author

Hyams C, Trzcinski K, Camberlein E, Weinberger DM, Chimalapati S, Noursadeghi M, Lipsitch M, and Brown JS

Subjects

Adult, Antibodies, Bacterial immunology, Antibodies, Bacterial metabolism, Bacterial Capsules metabolism, Bacterial Proteins immunology, Bacterial Proteins metabolism, Child, Complement C3 metabolism, Complement C3b metabolism, Complement Factor H metabolism, Humans, Mutation immunology, Neutrophils immunology, Neutrophils metabolism, Pneumococcal Infections metabolism, Protein Binding immunology, Serotyping methods, Streptococcus pneumoniae isolation & purification, Streptococcus pneumoniae metabolism, Streptococcus pneumoniae pathogenicity, Bacterial Capsules immunology, Complement C3 immunology, Complement C3b immunology, Complement Factor H immunology, Pneumococcal Infections immunology, Pneumococcal Infections microbiology, Streptococcus pneumoniae immunology

Abstract

Different capsular serotypes of Streptococcus pneumoniae vary markedly in their ability to cause invasive infection, but the reasons why are not known. As immunity to S. pneumoniae infection is highly complement dependent, variations in sensitivity to complement between S. pneumoniae capsular serotypes could affect invasiveness. We have used 20 capsule-switched variants of strain TIGR4 to investigate whether differences in the binding of the alternative pathway inhibitor factor H (FH) could be one mechanism causing variations in complement resistance and invasive potential between capsular serotypes. Flow cytometry assays were used to assess complement factor binding and complement-dependent neutrophil association for the TIGR4 capsule-switched strains. FH binding varied with the serotype and inversely correlated with the results of factor B binding, C3b/iC3b deposition, and neutrophil association. Differences between strains in FH binding were lost when assays were repeated with pspC mutant strains, and loss of PspC also reduced differences in C3b/iC3b deposition between strains. Median FH binding was high in capsule-switched mutant strains expressing more invasive serotypes, and a principal component analysis demonstrated a strong correlation between serotype invasiveness, high FH binding, and resistance to complement and neutrophil association. Further data obtained with 33 clinical strains also demonstrated that FH binding negatively correlated with C3b/iC3b deposition and that median FH binding was high in strains expressing more invasive serotypes. These data suggest that variations in complement resistance between S. pneumoniae strains and the association of a serotype with invasiveness could be related to capsular serotype effects on FH binding.

Published

2013

19. 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

20. Novel C3 mutation p.Lys65Gln in aHUS affects complement factor H binding.

Author

Volokhina E, Westra D, Xue X, Gros P, van de Kar N, and van den Heuvel L

Subjects

Adolescent, Adult, Amino Acid Sequence, Atypical Hemolytic Uremic Syndrome, Base Sequence, Child, Child, Preschool, Complement C3 chemistry, Complement C3b metabolism, Complement Factor H metabolism, DNA Mutational Analysis, Female, Hemolytic-Uremic Syndrome blood, Humans, Infant, Male, Middle Aged, Molecular Sequence Data, Protein Binding, Young Adult, Complement C3 genetics, Hemolytic-Uremic Syndrome genetics, Mutation, Missense

Abstract

Background: Atypical hemolytic uremic syndrome (aHUS) is associated with mutations affecting complement proteins and regulators and with autoantibodies against complement factor H (CFH). Approximately half of the aHUS patients progress to end-stage renal disease. DNA analysis of the risk factor genes is important for prognosis of aHUS recurrence after renal transplantation., Methods: Mutational screening of C3 encoding the central complement component was performed by Sanger sequencing in 70 aHUS patients. Mutated and wild type recombinant C3b proteins were produced and their affinity to CFH was analyzed by ELISA., Results: A single novel missense change p.Lys65Gln in C3 was found in 3 aHUS patients. The alteration leads to decreased binding of C3b to CFH in vitro. All three patients acquired the illness as adults and had a first aHUS episode after renal transplantation or suffered recurrence of the disease after transplantation., Conclusions: The novel C3 change was found in 3 aHUS patients. It results in decreased C3b binding to CFH and thus might lead to impaired C3b inactivation in vivo. The p.Lys65Gln is likely to be associated with aHUS after kidney transplantation and, therefore, might be an important prognostic factor.

Published

2012

21. Conformational states of a bacterial α2-macroglobulin resemble those of human complement C3.

Author

Neves D, Estrozi LF, Job V, Gabel F, Schoehn G, and Dessen A

Subjects

Bacterial Proteins metabolism, Bacterial Proteins ultrastructure, Complement C3 metabolism, Complement C3b chemistry, Complement C3b metabolism, Humans, Models, Molecular, Protein Conformation, alpha-Macroglobulins metabolism, alpha-Macroglobulins ultrastructure, Bacterial Proteins chemistry, Complement C3 chemistry, alpha-Macroglobulins chemistry

Abstract

α(2) macroglobulins (α(2)Ms) are broad-spectrum protease inhibitors that play essential roles in the innate immune system of eukaryotic species. These large, multi-domain proteins are characterized by a broad-spectrum bait region and an internal thioester, which, upon cleavage, becomes covalently associated to the target protease, allowing its entrapment by a large conformational modification. Notably, α(2)Ms are part of a larger protein superfamily that includes proteins of the complement system, such as C3, a multi-domain macromolecule which is also characterized by an internal thioester-carrying domain and whose activation represents the pivotal step in the complement cascade. Recently, α(2)M/C3-like genes were identified in a large number of bacterial genomes, and the Escherichia coli α(2)M homolog (ECAM) was shown to be activated by proteases. In this work, we have structurally characterized ECAM by electron microscopy and small angle scattering (SAXS) techniques. ECAM is an elongated, flexible molecule with overall similarities to C3 in its inactive form; activation by methylamine, chymotrypsin, or elastase induces a conformational modification reminiscent of the one undergone by the transformation of C3 into its active form, C3b. In addition, the proposed C-terminus of ECAM displays high flexibility and different conformations, and could be the recognition site for partner macromolecules. This work sheds light on a potential bacterial defense mechanism that mimics structural rearrangements essential for activation of the complement cascade in eukaryotes, and represents a possible novel target for the development of antibacterials.

Published

2012

22. Staphylococcus aureus proteins Sbi and Efb recruit human plasmin to degrade complement C3 and C3b.

Author

Koch TK, Reuter M, Barthel D, Böhm S, van den Elsen J, Kraiczy P, Zipfel PF, and Skerka C

Subjects

Blotting, Western, Cloning, Molecular, DNA Primers genetics, Enzyme-Linked Immunosorbent Assay, Humans, Plasminogen metabolism, Proteolysis, Surface Plasmon Resonance, Bacterial Proteins metabolism, Carrier Proteins metabolism, Complement C3 metabolism, Complement C3b metabolism, Complement Inactivator Proteins metabolism, Fibrinolysin metabolism, Immunity, Innate immunology, Staphylococcus aureus immunology

Abstract

Upon host infection, the human pathogenic microbe Staphylococcus aureus (S. aureus) immediately faces innate immune reactions such as the activated complement system. Here, a novel innate immune evasion strategy of S. aureus is described. The staphylococcal proteins surface immunoglobulin-binding protein (Sbi) and extracellular fibrinogen-binding protein (Efb) bind C3/C3b simultaneously with plasminogen. Bound plasminogen is converted by bacterial activator staphylokinase or by host-specific urokinase-type plasminogen activator to plasmin, which in turn leads to degradation of complement C3 and C3b. Efb and to a lesser extend Sbi enhance plasmin cleavage of C3/C3b, an effect which is explained by a conformational change in C3/C3b induced by Sbi and Efb. Furthermore, bound plasmin also degrades C3a, which exerts anaphylatoxic and antimicrobial activities. Thus, S. aureus Sbi and Efb comprise platforms to recruit plasmin(ogen) together with C3 and its activation product C3b for efficient degradation of these complement components in the local microbial environment and to protect S. aureus from host innate immune reactions.

Published

2012

23. β₂-glycoprotein I, the major target in antiphospholipid syndrome, is a special human complement regulator.

Author

Gropp K, Weber N, Reuter M, Micklisch S, Kopka I, Hallström T, and Skerka C

Subjects

Antiphospholipid Syndrome physiopathology, Apoptosis, Blotting, Western, Complement Activation, Complement C3 metabolism, Complement C3-C5 Convertases metabolism, Complement C3b metabolism, Complement Factor H metabolism, Humans, Immunoprecipitation, Molecular Conformation, Protein Binding, Recombinant Proteins immunology, Recombinant Proteins metabolism, beta 2-Glycoprotein I immunology, Antiphospholipid Syndrome immunology, Autoantibodies immunology, Complement C3 immunology, Complement C3b immunology, beta 2-Glycoprotein I metabolism

Abstract

The human plasma protein β(2)-glycoprotein I (β(2)-GPI) is the major target of autoantibodies associated with antiphospholipid syndrome. However, the biologic function of this abundant protein is still unclear. Here we identify β(2)-GPI as a complement regulator. β(2)-GPI circulates in the plasma in an inactive circular form. On surface binding, such as to apoptotic cells, β(2)-GPI changes conformation to an elongated form that acquires C3/C3b binding activities. β(2)-GPI apparently changes conformation of C3, so that the regulator factor H attaches and induces subsequent degradation by the protease factor I. β(2)-GPI also mediates further cleavage of C3/C3b compared with factor H alone. Our data provide important insights into innate immune regulation by plasma protein β(2)-GPI, which may be exploited in the prevention and therapy of autoimmune disease antiphospholipid syndrome.

Published

2011

24. Staphylococcus aureus metalloprotease aureolysin cleaves complement C3 to mediate immune evasion.

Author

Laarman AJ, Ruyken M, Malone CL, van Strijp JA, Horswill AR, and Rooijakkers SH

Subjects

Bacterial Proteins genetics, Bacterial Proteins metabolism, Blotting, Western, Complement Activation immunology, Complement C3 metabolism, Complement C3-C5 Convertases immunology, Complement C3-C5 Convertases metabolism, Complement C3a immunology, Complement C3a metabolism, Complement C3b immunology, Complement C3b metabolism, Cytotoxicity, Immunologic immunology, Host-Pathogen Interactions immunology, Humans, Metalloendopeptidases genetics, Metalloendopeptidases metabolism, Mutation, Neutrophils immunology, Phagocytosis immunology, Staphylococcal Infections microbiology, Staphylococcus aureus enzymology, Staphylococcus aureus physiology, U937 Cells, Bacterial Proteins immunology, Complement C3 immunology, Immune Evasion immunology, Metalloendopeptidases immunology, Staphylococcal Infections immunology, Staphylococcus aureus immunology

Abstract

Complement is one of the first host defense barriers against bacteria. Activated complement attracts neutrophils to the site of infection and opsonizes bacteria to facilitate phagocytosis. The human pathogen Staphylococcus aureus has successfully developed ways to evade the complement system, for example by secretion of specific complement inhibitors. However, the influence of S. aureus proteases on the host complement system is still poorly understood. In this study, we identify the metalloprotease aureolysin as a potent complement inhibitor. Aureolysin effectively inhibits phagocytosis and killing of bacteria by neutrophils. Furthermore, we show that aureolysin inhibits the deposition of C3b on bacterial surfaces and the release of the chemoattractant C5a. Cleavage analyses show that aureolysin cleaves the central complement protein C3. Strikingly, there was a clear difference between the cleavages of C3 in serum versus purified conditions. Aureolysin cleaves purified C3 specifically in the α-chain, close to the C3 convertase cleavage site, yielding active C3a and C3b. However, in serum we observe that the aureolysin-generated C3b is further degraded by host factors. We pinpointed these factors to be factor H and factor I. Using an aureolysin mutant in S. aureus USA300, we show that aureolysin is essential and sufficient for C3 cleavage by bacterial supernatant. In short, aureolysin acts in synergy with host regulators to inactivate C3 thereby effectively dampening the host immune response.

Published

2011

25. 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

26. Self-association and domain rearrangements between complement C3 and C3u provide insight into the activation mechanism of C3.

Author

Li K, Gor J, and Perkins SJ

Subjects

Complement C3 metabolism, Complement C3b chemistry, Complement C3b metabolism, Crystallography, X-Ray, Dimerization, Humans, Models, Molecular, Protein Conformation, Protein Structure, Tertiary, Ultracentrifugation, Complement C3 chemistry

Abstract

Component C3 is the central protein of the complement system. During complement activation, the thioester group in C3 is slowly hydrolysed to form C3u, then the presence of C3u enables the rapid conversion of C3 into functionally active C3b. C3u shows functional similarities to C3b. To clarify this mechanism, the self-association properties and solution structures of C3 and C3u were determined using analytical ultracentrifugation and X-ray scattering. Sedimentation coefficients identified two different dimerization events in both proteins. A fast dimerization was observed in 50 mM NaCl but not in 137 mM NaCl. Low amounts of a slow dimerization was observed for C3u and C3 in both buffers. The X-ray radius of gyration RG values were unchanged for both C3 and C3u in 137 mM NaCl, but depend on concentration in 50 mM NaCl. The C3 crystal structure gave good X-ray fits for C3 in 137 mM NaCl. By randomization of the TED (thioester-containing domain)/CUB (for complement protein subcomponents C1r/C1s, urchin embryonic growth factor and bone morphogenetic protein 1) domains in the C3b crystal structure, X-ray fits showed that the TED/CUB domains in C3u are extended and differ from the more compact arrangement of C3b. This TED/CUB conformation is intermediate between those of C3 and C3b. The greater exposure of the TED domain in C3u (which possesses the hydrolysed reactive thioester) accounts for the greater self-association of C3u in low-salt conditions. This conformational variability of the TED/CUB domains would facilitate their interactions with a broad range of antigenic surfaces. The second dimerization of C3 and C3u may correspond to a dimer observed in one of the crystal structures of C3b.

Published

2010

27. 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

28. Complement component C3 functions as an embryotrophic factor in early postimplantation rat embryos.

Author

Usami M, Mitsunaga K, Miyajima A, Sunouchi M, and Doi O

Subjects

Amino Acid Sequence, Animals, Binding, Competitive, Blotting, Western, Complement C3 metabolism, Complement C3b metabolism, Complement C3b pharmacology, Culture Media pharmacology, Embryo Culture Techniques, Embryo, Mammalian embryology, Embryo, Mammalian metabolism, Female, Immunohistochemistry, Male, Microscopy, Confocal, Molecular Sequence Data, Pregnancy, Protein Binding, Rabbits, Rats, Rats, Wistar, Time Factors, Yolk Sac embryology, Yolk Sac metabolism, Complement C3 pharmacology, Embryo, Mammalian drug effects, Embryonic Development drug effects

Abstract

A presumed embryotrophic factor for early postimplantation rat embryos, partially purified from rat serum, was identified as complement component C3 (C3), the central component of the complement system, by sequence analysis of its N-terminal. Purified rat C3 showed embryotrophic activity for rat embryos cultured from day 9.5 of gestation for 48 h in the culture medium composed of rabbit serum. The maximum embryotrophic activity of C3 was observed around 0.5 mg/ml, a level which is lower than rat serum C3 levels. In the culture medium composed of rat serum, cultured rat embryos selectively consumed C3, and C3-depletion by cobra venom factor affected embryonic growth. Inactivation of the internal thiolester bond of C3, the critical functional site for its activity in the complement system, by methylamine had no effects on its embryotrophic activity. Purified rabbit C3 had only weak embryotrophic activity for cultured rat embryos, suggesting species specificity of the embryotrophic activity of C3. Immunochemical analyses showed the specific presence of C3 on the visceral yolk sac, but not on the embryo proper of day 9.5 or 10.5 rat embryos both in utero and in vitro. In analysis using fluorescein-labeled rat C3, unfragmented C3s bound to the visceral yolk sac stronger than C3b, the primary active fragment of C3 in the complement system. These results indicate that C3, which has always been considered to be detrimental to embryos, functions as an embryotrophic factor by novel mechanisms probably through the visceral yolk sac. The present study thus provides new insights into functions of C3 and postimplantation embryonic growth.

Published

2010

29. Regulation of complement-3 protein expression in human and mouse oviducts.

Author

Lee YL, Cheong AW, Chow WN, Lee KF, and Yeung WS

Subjects

Analysis of Variance, Animals, Cell Line, Complement C3 genetics, Complement C3b metabolism, Estrogens blood, Estrogens metabolism, Estrogens pharmacology, Fallopian Tubes cytology, Female, Gene Expression Regulation drug effects, Humans, Male, Mice, Ovariectomy, Pregnancy, Progesterone blood, Progesterone metabolism, Progesterone pharmacology, Pseudopregnancy metabolism, Complement C3 metabolism, Fallopian Tubes metabolism, Gene Expression Regulation physiology

Abstract

The human oviduct derived embryotrophic factor-3 (ETF-3) contains complement protein-3 (C3) and its derivates. Although C3 is not embryotrophic, it is converted into the embryotrophic derivative, iC3b in the presence of embryos and oviductal cells. The regulation of C3 production in the oviduct is not known. The objectives of this study were to investigate the effects of presence of preimplantation embryos and hormones on C3 expression in the oviducts in vitro and in vivo. The expression of C3 in the oviduct of pregnant mice was compared to that of pseudo-pregnant mice. The hormonal action on C3 expression was studied in the ovariectomized mouse oviducts and human oviductal epithelial (OE) cells. The results showed that the level of C3 mRNA in the mouse oviduct was high on Day 1 and Day 2, but decreased to a minimum on Day 4 of pregnancy, whereas that of pseudo-pregnancy remained relatively stable within the same period. The protein levels of C3 and iC3b specific fragments, alpha-115 and alpha-40, respectively in the mouse oviductal luminal fluid were highest on Day 3 of pregnancy, when the embryos were expected to be most sensitive to the embryotrophic activity of ETF-3. Estrogen elevated C3 expression in the ovariectomized mouse oviduct and the OE cells. Progesterone suppressed estrogen-induced C3 expression in the mouse oviduct, but had no effect on OE cells. In conclusion, the presence of embryo and steroid hormones regulate the synthesis and secretion of oviductal C3.

Published

2009

30. Immune evasion of Enterococcus faecalis by an extracellular gelatinase that cleaves C3 and iC3b.

Author

Park SY, Shin YP, Kim CH, Park HJ, Seong YS, Kim BS, Seo SJ, and Lee IH

Subjects

Amino Acid Sequence, Animals, Blood Bactericidal Activity immunology, Chickens, Complement Activation immunology, Complement C3 antagonists & inhibitors, Complement C3 physiology, Complement C3b antagonists & inhibitors, Complement Pathway, Alternative immunology, Dogs, Extracellular Fluid immunology, Gram-Positive Bacterial Infections enzymology, Gram-Positive Bacterial Infections immunology, Gram-Positive Bacterial Infections microbiology, Guinea Pigs, Humans, Hydrolysis, Mice, Molecular Sequence Data, Neutrophils immunology, Phagocytosis immunology, Complement C3 metabolism, Complement C3b metabolism, Enterococcus faecalis enzymology, Enterococcus faecalis immunology, Extracellular Fluid enzymology, Gelatinases physiology

Abstract

Enterococcus faecalis (Ef) accounts for most cases of enterococcal bacteremia, which is one of the principal causes of nosocomial bloodstream infections (BSI). Among several virulence factors associated with the pathogenesis of Ef, an extracellular gelatinase (GelE) has been known to be the most common factor, although its virulence mechanisms, especially in association with human BSI, have yet to be demonstrated. In this study, we describe the complement resistance mechanism of Ef mediated by GelE. Using purified GelE, we determined that it cleaved the C3 occurring in human serum into a C3b-like molecule, which was inactivated rapidly via reaction with water. This C3 convertase-like activity of GelE was shown to result in a consumption of C3 and thus inhibited the activation of the complement system. Also, GelE was confirmed to degrade an iC3b that was deposited on the Ag surfaces without affecting the bound C3b. This proteolytic effect of GelE against the major complement opsonin resulted in a substantial reduction in Ef phagocytosis by human polymorphonuclear leukocytes. In addition, we verified that the action of GelE against C3, which is a central component of the complement cascade, was human specific. Taken together, it was suggested that GelE may represent a promising molecule for targeting human BSI associated with Ef.

Published

2008

31. Phosphorylation of C3 by a casein kinase released from activated human platelets increases opsonization of immune complexes and binding to complement receptor type 1.

Author

Nilsson-Ekdahl K and Nilsson B

Subjects

Biotinylation, Blood Platelets metabolism, Casein Kinases, Complement C3 immunology, Complement C3b immunology, Complement C3b metabolism, Complement Factor B metabolism, Complement Factor H metabolism, Complement Pathway, Alternative, Erythrocytes immunology, Erythrocytes metabolism, Fibrinogen metabolism, Hot Temperature, Humans, Immunoglobulin G immunology, Immunoglobulin G metabolism, Phosphorylation, Protein Binding, Recombinant Proteins metabolism, Solubility, gamma-Globulins immunology, gamma-Globulins metabolism, Antigen-Antibody Complex immunology, Blood Platelets enzymology, Complement C3 metabolism, Opsonin Proteins immunology, Platelet Activation, Protein Kinases metabolism, Receptors, Complement metabolism

Abstract

We have previously demonstrated that complement component C3 is phosphorylated both in vitro and in vivo by a casein kinase released from activated human platelets. In vitro, the studies have shown that cleavage of C3b by factor I is decreased, and binding to various target surfaces is enhanced by affecting the thiol ester. In the present study we have examined the effect of phosphorylation on the binding of C3b to complement receptor 1 (CR1, CD35). Upon phosphorylation by platelet casein kinase, C3b covalently bound to activated thiol Sepharose bound higher amounts of soluble recombinant CR1. Similar effects were demonstrated with two ELISA systems in which microtiter plates were coated with phosphorylated or unphosphorylated purified C3b or with C3 activated by the alternative pathway convertase. Phosphorylated C3b was also four times more efficient than unphosphorylated C3b in inhibiting the binding of complement-opsonized human aggregated gammaglobulin to erythrocytes. A similar increase in binding was found at low serum concentrations when the C3 activation occurred in C3-deficient serum reconstituted with phosphorylated or unphosphorylated C3. In this serum system, using a monoclonal antibody specific for iC3b, we also demonstrated that the phosphorylated C3b was protected against cleavage to iC3b. Corresponding experiments using factor H showed a decrease in binding of both fluid-phase and bound C3b to factor H. We postulate that phosphorylation of C3 by activated platelets amplifies the complement-mediated binding of immune complexes to CR1 by three different mechanisms: decreased cleavage of C3b to iC3b, increased deposition of C3b to immune complexes, and increased binding of C3b to CR1.

Published

2001

32. Complement-dependent proinflammatory properties of the Alzheimer's disease beta-peptide.

Author

Bradt BM, Kolb WP, and Cooper NR

Subjects

Animals, Complement C5b, Humans, Rabbits, Alzheimer Disease metabolism, Amyloid beta-Peptides metabolism, Complement C3 metabolism, Complement C3b metabolism, Complement C5 metabolism, Complement C5a metabolism, Peptide Fragments metabolism

Abstract

Large numbers of neuritic plaques (NP), largely composed of a fibrillar insoluble form of the beta-amyloid peptide (Abeta), are found in the hippocampus and neocortex of Alzheimer's disease (AD) patients in association with damaged neuronal processes, increased numbers of activated astrocytes and microglia, and several proteins including the components of the proinflammatory complement system. These studies address the hypothesis that the activated complement system mediates the cellular changes that surround fibrillar Abeta deposits in NP. We report that Abeta peptides directly and independently activate the alternative complement pathway as well as the classical complement pathway; trigger the formation of covalent, ester-linked complexes of Abeta with activation products of the third complement component (C3); generate the cytokine-like C5a complement-activation fragment; and mediate formation of the proinflammatory C5b-9 membrane attack complex, in functionally active form able to insert into and permeabilize the membrane of neuronal precursor cells. These findings provide inflammation-based mechanisms to account for the presence of complement components in NP in association with damaged neurons and increased numbers of activated glial cells, and they have potential implications for the therapy of AD.

Published

1998

33. The C(H)1 domain of IgG is not essential for C3 covalent binding: importance of the other constant domains as targets for C3.

Author

Muñoz E, Vidarte L, Casado MT, Pastor C, and Vivanco F

Subjects

Animals, Complement C3b metabolism, Electrophoresis, Gel, Two-Dimensional, Humans, Hybridomas, Macromolecular Substances, Mice, Protein Binding, Rabbits, Recombinant Fusion Proteins, Recombinant Proteins, Antigen-Antibody Complex metabolism, Complement C3 metabolism, Immunoglobulin Constant Regions metabolism, Immunoglobulin Heavy Chains metabolism

Abstract

The covalent binding of C3 to antigen-antibody complexes [immune complexes (IC)] plays a pivotal role in the elimination of antigens. C3 prevents the formation of large IC lattices promoting their solubilization. Subsequently, bound C3 fragments determine the efficacy of antigen presentation, and the generation of antibody responses and immunological memory. C3 binding to IgG-IC generates IgG-C3b-C3b complexes which are detected by SDS-PAGE as two major bands: C3alpha65-heavy chain and C3alpha65-C3alpha43 covalent complexes. Using human heat-aggregated IgG1 as a model of IC, a C3b binding site was localized only in the Cgamma1 domain. However, with true IC of ovalbumin and rabbit IgG anti-ovalbumin, C3b binds to both the Fab and Fc regions of IgG. To study the binding of C3b to the different domains of IgG and particularly to evaluate the involvement of the Cgamma1 domain, we have constructed recombinant single-chain antibodies without Cgamma1, which have the structure: V(H)-linker-V(L)-hinge-Cgamma2-Cgamma3 (scAb). The variable domains were from a mouse mAb anti-HSA and the constant region (hinge-C(H)2-C(H)3) from human IgG1 or rabbit IgG. C3 binds very efficiently to IC formed with human (h-scAb) or rabbit (r-scAb) recombinant antibodies (scAb-HSA) and generates also two bands on SDS-PAGE (C3alpha65-scAb and C3alpha65-C3alpha43), which are the counterparts of those of the complete antibody. In addition, IC formed with scAb activate the alternative pathway to a similar extent as IC of the entire IgG. These data indicate that the Cgamma1 domain is a dispensable region for C3b binding and that the remaining constant domains are as efficient as Cgamma1 in C3b binding. Overall these results support the view that C3 does not specifically recognize a unique site in the Cgamma1 domain. Rather it seems to be able to attach along the antibody molecule. Probably this implies an advantage for effective processing of C3b-IC and elimination of antigens in vivo.

Published

1998

34. The requirement of localized, CR2-mediated, alternative pathway activation of complement for covalent deposition of C3 fragments on normal B cells.

Author

Olesen EH, Johnson AA, Damgaard G, and Leslie RG

Subjects

Blotting, Western, Cell Culture Techniques, Complement C3b biosynthesis, Complement C3b metabolism, Dose-Response Relationship, Immunologic, Electrophoresis, Polyacrylamide Gel, Humans, Peptide Fragments metabolism, B-Lymphocytes immunology, Complement C3 metabolism, Complement Pathway, Alternative immunology, Receptors, Complement 3d immunology

Abstract

We have shown previously that normal B cells share, with Epstein-Barr virus-transformed and malignant B cells, the ability to activate the alternative pathway (AP) of complement in vitro, resulting in the deposition of C3 fragments on the cell surface. Complement receptor type 2 (CR2, CD21) has been implicated directly as the site for formation of an AP convertase, which provides nascent C3b for deposition at secondary sites on the B-cell surface. In the present study, we have examined C3 fragment deposition in vitro in more detail by (1) assessing the importance of locally generated C3b for the deposition process, (2) investigating whether CR2 is the sole requirement for conferring AP activation capacity on a cell, and (3) determining whether CR2's function, as an AP activator, has different structural requirements from ligand binding. Increasing the availability of native C3, by increasing the serum (NHS) concentration, resulted in enhanced C3 fragment deposition on the B cells, whereas use of factor 1-depleted NHS, which showed massive fluid phase C3 conversion during the incubation, diminished the deposition. Sodium dodecyl sulphate-polyacrylamide gel electrophoresis (SDS-PAGE) and Western blotting of untreated and hydroxylamine-treated lysates from B cells, after in vitro activation, revealed that the majority of C3 fragments (primarily iC3b and C3dg) had been covalently bound to the cell surface. Transfection of COS cells with wild-type CR2 or a deletion mutant lacking 11 of the molecule's 15 homologous domains, but retaining the ligand-binding site, revealed that expression of intact CR2 conferred a 12-fold increase in AP-activating capacity on these cells, while no increase in AP activity was apparent on cells transfected with the mutant CR2.

Published

1998

35. Complement factor C3 deposition and serum resistance in isogenic capsule and lipooligosaccharide sialic acid mutants of serogroup B Neisseria meningitidis.

Author

Vogel U, Weinberger A, Frank R, Müller A, Köhl J, Atkinson JP, and Frosch M

Subjects

Bacterial Capsules genetics, Complement C3b metabolism, Humans, Mutation, N-Acetylneuraminic Acid genetics, Sialyltransferases genetics, UDPglucose 4-Epimerase genetics, Bacterial Capsules immunology, Blood Bactericidal Activity, Complement C3 metabolism, Lipopolysaccharides immunology, N-Acetylneuraminic Acid immunology, Neisseria meningitidis immunology

Abstract

Serogroup B meningococci express sialic acids on their surfaces as a modification of the lipooligosaccharide (LOS) and as capsular material consisting of alpha2,8-linked sialic acid homopolymers. The aim of this study was to elucidate the impact of each sialic acid component on the deposition of complement factor C3 and serum resistance. For this purpose, we used isogenic mutants deficient in capsule expression (a polysialyltransferase mutant) or sialylation of the LOS (a galE mutant) or both (a mutant with a deletion of the cps gene locus). Bactericidal assays using 40% normal human serum (NHS) demonstrated that both the capsule and LOS sialic acid are indispensable for serum resistance. By immunoblotting with monoclonal antibody MAb755 that is specific for the C3 alpha-chain, we were able to demonstrate that C3 from 40% NHS was covalently linked to the surface structures of meningococci as C3b and iC3b, irrespective of the surface sialic acid compounds. However, C3b linkage was more pronounced and occurred on a larger number of target molecules in galE mutants with nonsialylated LOS than in meningococci with wild-type LOS, irrespective of the capsule phenotype. C3b deposition was caused by both the classical pathway (CP) and the alternative pathway of complement activation. Use of 10% NHS revealed that at low serum concentrations, C3 deposition occurred via the CP and was detected primarily on nonsialylated-LOS galE mutants, irrespective of the capsular phenotype. Accordingly, immunoglobulin M (IgM) binding to meningococci from heat-inactivated NHS was demonstrated only in both encapsulated and unencapsulated galE mutants. In contrast, inhibition of IgA binding required both encapsulation and LOS sialylation. We conclude that serum resistance in wild-type serogroup B meningococci can only be partly explained by an alteration of the C3b linkage pattern, which seems to depend primarily on the presence of wild-type LOS, since a serum-resistant phenotype also requires capsule expression.

Published

1997

36. Cleavage of the complement system C3 component by HIV-1 proteinase.

Author

Kisselev AF, Mentele R, and von der Helm K

Subjects

Amino Acids metabolism, Binding Sites, Complement Activation drug effects, Complement Activation genetics, Complement C3b genetics, Complement C3c genetics, Complement C3d genetics, Electrophoresis, Polyacrylamide Gel, HIV Protease pharmacology, Humans, In Vitro Techniques, Molecular Weight, Complement C3 metabolism, Complement C3b metabolism, Complement C3c metabolism, Complement C3d metabolism, HIV Protease metabolism

Abstract

The C3 factor of the complement system and its C3b fragment are cleaved in vitro by the proteinase of the human immunodeficiency virus, type 1 (HIV PR). The cleavage occurs in the alpha-chain of both substrates at multiple sites yielding a 100 kDa fragment of the C3 alpha-chain and multiple fragments of the C3b alpha-chain. The scissile bonds are: Ala86-Glu87, Leu310-Leu311, His641-Trp642 and Arg649-Ser650. The resulting fragments resemble the physiologically occurring inactive fragments of C3: C3c and C3d, suggesting a possible biological role of the HIV-proteinase in the complement inactivation process.

Published

1997

37. Activation, binding, and processing of complement component 3 (C3) by Blastomyces dermatitidis.

Author

Zhang MX and Klein B

Subjects

Complement C3b immunology, Complement C3b metabolism, Egtazic Acid pharmacology, Electrophoresis, Polyacrylamide Gel, Flow Cytometry, Fluorescent Antibody Technique, Indirect, Glucans pharmacology, Humans, Hydroxylamine, Hydroxylamines pharmacology, Immunoglobulins blood, Immunoglobulins metabolism, Immunoglobulins pharmacology, Kinetics, Opsonin Proteins immunology, Time Factors, Blastomyces immunology, Blastomyces metabolism, Complement C3 immunology, Complement C3 metabolism, Complement Pathway, Alternative immunology, Complement Pathway, Classical immunology, Protein Binding

Abstract

Complement plays a key role in phagocyte recognition and killing of Blastomyces dermatitidis, but little is known about how complement components interact with the yeast. We report the characteristics of activation, binding, and processing of C3 by B. dermatitidis. In pooled normal human serum (NHS), deposition of C3 on the yeast was detectable within 2 min, whereas in NHS containing MgEGTA, deposition was delayed by 6 min, indicating that the yeast activates C3 by both classical and alternative pathways. When both pathways were operative, maximal binding of 4.5 x 10(6) C3 molecules/cell was achieved in less than 30 min. In the absence of the classical pathway, yeast cells bound 80% of the maximum C3, indicating that the yeast intrinsically activates the alternative pathway. Delayed deposition of C3 in NHS-MgEGTA was similar to that in NHS preabsorbed by the yeast or by immobilized protein A/G to remove serum immunoglobulin. Purified immunoglobulin restored C3 binding to NHS preabsorbed by the yeast, suggesting that antibody in nonimmune serum initiates the classical pathway. beta-Glucan absorption of NHS abolished the classical pathway, suggesting that cell wall beta-glucan is a target of initiating antibodies. Hydroxylamine treatment of NHS-opsonized yeast cells showed that 76% of C3 was bound to yeast cells by ester linkage, supporting a role for hydroxyl groups on cell wall polysaccharides. Hydroxylamine-cleaved fragments were chiefly C3b and iC3b; 70% of hydroxylamine-sensitive C3b was converted to iC3b within 1 min of opsonization, and the ratio was stable over 1 h. Our data predict that C3b and iC3b on opsonized yeast cells direct binding to CR1 and CR3 receptors on human phagocytes, which, in turn, may influence the fate of this host-pathogen interaction.

Published

1997

38. Analysis of complement C3 deposition and degradation on Klebsiella pneumoniae.

Author

Albertí S, Alvarez D, Merino S, Casado MT, Vivanco F, Tomás JM, and Benedí VJ

Subjects

Blood, Blotting, Western, Humans, Lipopolysaccharides immunology, Opsonin Proteins, Porins immunology, Porins metabolism, Bacterial Proteins, Complement C3 metabolism, Complement C3b metabolism, Complement Pathway, Alternative, Complement Pathway, Classical, Klebsiella pneumoniae immunology

Abstract

The majority of Klebsiella pneumoniae serum-resistant strains activate complement and bind C3b, the opsonic fragment of C3, without C5b-9 formation and bacterial killing. The mechanisms leading to C3b deposition without cell death were studied, and the results indicate that serum-resistant strains activate principally the alternative pathway and that serum-sensitive strains activate both the alternative and classical pathways. Bacterial molecules implicated in C3b deposition are the outer membrane porin proteins and smooth and rough lipopolysaccharides. Porins activate both complement pathways, and the rough lipopolysaccharide activates the classical pathway, causing deposition of C3b in serum-sensitive strains. The smooth lipopolysaccharide of serum-resistant strains activates only the alternative pathway, impeding the binding of C1q to porins (S. Albertí, G. Marqués, S. Camprubí, S. Merino, J. M. Tomás, F. Vivanco, and V. J. Benedí, Infect. Immun. 61:852-860, 1993; S. Albertí, F. Rodríguez-Quinónes, T. Schirmer, G. Rummel, J. M. Tomás, J. P. Rosenbusch, and V. J. Benedí, Infect. Immun. 63:903-910, 1995) and rough lipopolysaccharide molecules and thereby preventing activation of the classical pathway. After its deposition, C3b is quickly degraded to iC3b on both types of strains, but the higher-level deposition of C3b on serum-sensitive strains, resulting from activation of both the alternative and classical complement pathways, supports further complement activation and killing of serum-sensitive strains.

Published

1996

39. Inhibition of human complement by a C3-binding peptide isolated from a phage-displayed random peptide library.

Author

Sahu A, Kay BK, and Lambris JD

Subjects

Amino Acid Sequence, Bacteriophages isolation & purification, Binding, Competitive immunology, Complement Activation drug effects, Complement C3 drug effects, Complement C3-C5 Convertases antagonists & inhibitors, Complement C3-C5 Convertases pharmacology, Complement C3b metabolism, Complement Factor B metabolism, Gene Library, Humans, Molecular Sequence Data, Properdin metabolism, Protein Binding immunology, Bacteriophages genetics, Bacteriophages metabolism, Complement C3 metabolism, Complement Inactivator Proteins isolation & purification, Complement Inactivator Proteins pharmacology, Peptides isolation & purification, Peptides pharmacology

Abstract

We have screened a phage-displayed random peptide library for binding to C3b, the proteolytically activated form of complement component C3, and have identified a novel peptide that suppresses complement activation. This phage-displayed peptide bound to C3, C3b, and C3c, but not to C3d, indicating that it binds to the C3c region of C3. A synthetic 27-amino acid peptide corresponding to the phage-displayed peptide also bound to C3 and C3 fragments and inhibited both the classical and alternative pathways of complement activation. The inhibition of complement activation was reversible. Studies with overlapping peptides indicated that the functional activity was located in the cyclic 13-amino acid N-terminal region (ICVVQDWGHHRCT) of the parent peptide. Reduction and alkylation of this 13-residue synthetic peptide destroyed its inhibitory activity. Analysis of the mechanism of inhibition revealed that the peptide inhibited C3 cleavage in normal human serum as well as when the alternative pathway was reconstituted with purified complement components, and the observed inhibition was not due to sterically hindered access to the C3a/C3b cleavage site. Further, the peptide did not inhibit the cleavage of factor B, indicating that it did not affect the interaction of CA with factor B or the formation of C3b,Bb. The peptide also had no effect on the binding of properdin to C3, demonstrating that the observed inhibition of C3 cleavage in normal human serum was not due in part to its effect on the properdin-stabilized C3 convertase, C3b,Bb,P. These results indicate that the peptide we have identified interacts with C3 to inhibit its activation.

Published

1996

40. Investigation of mechanism-based inhibitors of complement targeting the activated thioester of human C3.

Author

Sahu A and Pangburn MK

Subjects

Humans, Hydroxylation, Phenols metabolism, Phenols pharmacology, Tyrosine analogs & derivatives, Tyrosine pharmacology, Complement C3 metabolism, Complement C3b metabolism, Complement C3b Inactivator Proteins pharmacology

Abstract

An intramolecular thioester bond in complement protein C3 is vital for covalent attachment of C3b (the proteolytically activated form of C3) to biological surfaces and for activation of the complement system. Proteolytic removal of C3a from C3 activates the thioester in the C3b fragment. Activated C3b primarily forms ester bonds with hydroxyl groups of carbohydrates on complement activating surfaces, but it has also been shown to react with the hydroxyl group of tyrosine and with specific Ser and Thr residues on IgG and on complement protein C4b. To examine the reactivity of the thioester, several families of hydroxylated compounds were examined. Reactivity of a series of substituted phenols varied over two orders of magnitude and demonstrated a linear correlation between reactivity and the Hammett substituent constants. Hydroxylated drugs including members of the L-DOPA/epinephrine family and hydroxamic acids also were examined. Compounds were identified that were 20,000 times more reactive than carbohydrates. These compounds were found to inhibit both the classical and alternative pathways of complement activation. Although the specificity of the thioester for its natural biological targets appears to be determined by many structural features, the data presented here demonstrate that increasing the nucleophilic character of the target hydroxyl group can increase the potency of a synthetic inhibitor many orders of magnitude.

Published

1996

41. Activation of complement in quails bearing Rous sarcoma virus-induced tumors.

Author

Kai C, Yoshikawa Y, and Yamanouchi K

Subjects

Animals, Complement C3b metabolism, Coturnix, Kinetics, Sarcoma, Avian blood, Time Factors, Avian Sarcoma Viruses, Complement Activation, Complement C3 metabolism, Sarcoma, Avian immunology

Abstract

The concentration of serum C3 in quails bearing tumors induced by Rous sarcoma virus (RSV) was elevated in parallel with tumor growth, whereas serum C3 levels in quails inoculated with avian leukosis virus, which lacks transforming activity, showed a pattern similar to that in mock-infected quails. C3 deposition was also observed in almost all tumor cells at the tumor developing stage. These findings obtained in vivo suggest that the cells transformed by RSV activated the C3 on their surfaces.

Published

1995

42. Phosphorylation of complement component C3 and C3 fragments by a human platelet protein kinase. Inhibition of factor I-mediated cleavage of C3b.

Author

Ekdahl KN and Nilsson B

Subjects

Binding Sites, Complement C3b metabolism, Complement Factor H metabolism, Complement Factor I metabolism, Humans, In Vitro Techniques, Peptide Fragments metabolism, Phosphorylation, Platelet Activation, gamma-Globulins pharmacology, Blood Platelets enzymology, Complement C3 metabolism, Protein Kinases metabolism

Abstract

Phosphorylation of C3 in vitro has been shown previously to lead to significantly altered function of the protein. Platelets are known to contain and release considerable amounts of protein kinases and ATP, which are prerequisites for protein phosphorylation. The aim of the present study was to investigate whether C3 is phosphorylated extracellularly by human platelets. Platelet-rich plasma was stimulated by human aggregated gamma-globulin or ADP. The remaining cells were removed by centrifugation, and the plasma was incubated with [gamma-32P]ATP. After precipitation with Sepharose-bound Abs to C3c followed by SDS-PAGE, it was shown that C3 was phosphorylated in the alpha-chain by a protein kinase dependent on Mn2+, Ca2+, or Mg2+ ions. The supernatant from washed, activated platelets was incubated with purified C3 or soluble or activated thiol Sepharose-bound C3b, together with [gamma-32P]ATP. Phosphorylation was seen in the alpha-chain of C3, and to the same extent in the alpha'-chain of both C3b preparations. The analysis of acid hydrolysate demonstrated that C3 contained 32P-labeled Thr and 32P-labeled Ser. After extensive proteolysis with trypsin, the major phosphorylation site was located to a peptide of 3 to 4 kDa that was bound to the activated thiol Sepharose via the free sulphydryl group in the C3d fragment. Incubation of phosphorylated C3b with factors I and H showed that phosphorylation inhibited the cleavage of the alpha'-chain of C3b. The results in this study suggest that phosphorylation is a regulator of C3 during platelet activation induced, for example, by immune complexes.

Published

1995

43. Interactions of human complement component C3 with factor B and with complement receptors type 1 (CR1, CD35) and type 3 (CR3, CD11b/CD18) involve an acidic sequence at the N-terminus of C3 alpha'-chain.

Author

Taniguchi-Sidle A and Isenman DE

Subjects

Amino Acid Sequence, Cell Line, Complement C3b metabolism, Complement Hemolytic Activity Assay, Humans, Molecular Sequence Data, Mutagenesis, Site-Directed, Protein Binding, Rosette Formation, Sequence Homology, Amino Acid, Complement C3 chemistry, Complement C3 metabolism, Complement Factor B metabolism, Receptors, Complement metabolism

Abstract

Complement component C3 is a multifunctional protein that interacts with many different ligands and receptors. Several experimental approaches involving blocking Abs, proteolytic fragmentation, and synthetic peptides have been used to predict which regions in C3 are required for its various functions. We have used site-directed mutagenesis to alter specific residues in the C3 segments 730-739 and 933-942 that have been proposed to be required for the binding of factor B by C3, and have examined, within the context of the intact C3b molecule, the effect of these substitutions on the C3b-factor B interaction. Because it has been suggested that factor H and complement receptors type 1, 2, and 3 may recognize sites in C3 that partially or completely overlap those of factor B, the relevant proteolytic fragment of each mutant C3 was tested for its ability to interact with these molecules. This study clearly demonstrates that a segment near the N-terminus of the alpha'-chain, which contains the negatively charged residues 730DE and 736EE, is involved in the interactions of C3 proteolytic fragments with factor B and complement receptors type 1 and 3, but not type 2. Factor H cofactor activity was also partially affected by these mutations. In contrast, mutation of the 937KED triplet in the C3 933-942 segment had little or no effect on any of these activities.

Published

1994

44. Bovine conglutinin binds to an oligosaccharide determinant presented by iC3b, but not by C3, C3b or C3c.

Author

Laursen SB, Thiel S, Teisner B, Holmskov U, Wang Y, Sim RB, and Jensenius JC

Subjects

Animals, Blotting, Western, Cattle, Complement C3 immunology, Complement C3b immunology, Complement C3b metabolism, Complement C3b Inactivator Proteins immunology, Complement C3c immunology, Complement C3c metabolism, Electrophoresis, Polyacrylamide Gel, Enzyme-Linked Immunosorbent Assay, Collectins, Complement C3 metabolism, Epitopes metabolism, Oligosaccharides metabolism, Serum Globulins metabolism

Abstract

Bovine conglutinin is a serum lectin that agglutinates erythrocytes preincubated with antibodies and complement. This agglutination occurs through the binding of conglutinin to iC3b, a fragment of the complement component C3. It was reported that conglutinin binds fluid-phase C3b and C3c as well as iC3b. We re-investigated the reactivity of conglutinin towards fluid-phase C3 degradation products. ELISA wells were coated with conglutinin and reacted with C3 split products generated in normal human serum, in factor I-deficient serum, or in factor I-depleted serum. Conglutinin-bound C3 fragments were detected with anti-C3c and anti-C3d antibodies. An increased signal was observed during the activation of complement in normal human serum with the peak response after 1-2 hr, following which the signal decreased, reaching background level after 72 hr. The oligosaccharides on C3c, generated in serum, are thus not recognized by conglutinin. No signal was observed when factor I-deficient serum or factor I-depleted serum was used instead of normal serum. Reconstitution with purified factor I re-established the normal pattern. Examination of the conglutinin-bound C3 molecules by SDS-PAGE and Western blotting with anti-C3c and anti-C3d antibodies revealed bands characteristic for iC3b, and no bands corresponding to C3b or C3c. Reduction of the disulphide bonds prior to the incubation of the activated serum with the conglutinin-coated wells revealed a band of 63,000 MW, characteristic of the N-terminal fragment of the alpha-chain of iC3b. We also investigated the binding to the solid-phase conglutinin of purified C3 and degradation products generated with enzymes. In this case, C3 as well as C3b and C3c were bound, suggesting conformational changes in C3 during purification. In conclusion, when C3 conversion takes place at near physiological conditions, conglutinin interacts specifically with the oligosaccharide on the alpha-chain of iC3b.

Published

1994

45. C3 binds with similar efficiency to Fab and Fc regions of IgG immune aggregates.

Author

Antón LC, Ruiz S, Barrio E, Marqués G, Sánchez A, and Vivanco F

Subjects

Animals, Antigen-Antibody Complex chemistry, Binding Sites, Complement C3b metabolism, Complement Pathway, Alternative, Hydroxylamine, Hydroxylamines chemistry, In Vitro Techniques, Macromolecular Substances, Peptide Mapping, Protein Binding, Rabbits, Antigen-Antibody Complex metabolism, Complement C3 metabolism, Immunoglobulin Fab Fragments metabolism, Immunoglobulin Fc Fragments metabolism

Abstract

The covalent binding reaction of the third component of complement (C3) with rabbit IgG immune aggregates has been studied by enzymic digestion of C3b-IgG adducts. In these adducts C3b was radioactively labeled in the free thiol group generated during activation of the internal thioester of C3. Trypsin digestion of 14C-labeled C3b-IgG adducts degrades C3b to a small antibody-bound 14C-labeled C3 fragment (14C-C3frg), whereas the antibody remains unaltered. Papain digestion of trypsin-treated 14C-C3frg-IgG complexes generated Fc and Fab fragments bearing equivalent amounts of covalently bound 14C-C3frg (43% and 40%, of the total C3 present in the aggregates, respectively). Hydroxylamine treatment of the 14C-C3frg-Fab and 14C-C3frg-Fc complexes released a 14C-C3frg of similar size (about 3-4 kDa) in which the N-terminal residue was the radiolabeled Cys1010. A fragment with the same radioactive N terminus and characteristics was obtained by sequential trypsin and papain digestion of purified C3 labeled with iodo-[14C] acetamide. Affinity-purified 14C-C3frg-Fc complexes digested with pepsin generated a mixture of radioactive peptides, most probably complexes formed by 14C-C3frg and C gamma 2 or the hinge digestion products, and 14C-C3frg-pFc' complexes. The latter was also immunoprecipitated with anti-Fc-Sepharose from the pepsin digestion supernatants of 14C-labeled-C3b-IgG complexes. Taken together these data indicate that, during complement activation through the alternative pathway by IgG immune aggregates, C3 is not bound to a single site on the antibody molecule. Both Fab and Fc regions of IgG are equally efficient targets for C3 anchorage. In addition, the data confirm the pFc' as a region of C3 attachment within the Fc portion, and strongly suggest that C3b is bound either to the C gamma 2 domain or the hinge or both.

Published

1994

46. The hemopoietic progenitor 32DCl3(G) cells synthesize C3 molecules and acquire C3b acceptor sites upon differentiation or neoplastic transformation.

Author

Di Renzo L, Zicari A, Longo A, Realacci M, Naso G, Pontieri G, and Lipari M

Subjects

Animals, Binding Sites, Cell Differentiation, Cell Line, Cell Transformation, Viral, Cells, Cultured, Complement Pathway, Alternative, Genes, ras, Hematopoiesis, Hematopoietic Stem Cells cytology, Mice, Mice, Inbred C3H, Cell Transformation, Neoplastic immunology, Complement C3 biosynthesis, Complement C3b metabolism, Hematopoietic Stem Cells metabolism

Abstract

32DCl3(G) cells are a diploid, nontumorigenic, IL-3-dependent hemopoietic progenitor cell line, which undergoes terminal differentiation into neutrophilic granulocytes when cultured in presence of G-CSF. The infection with BALB-Moloney murine sarcoma virus, containing a v-HA-ras oncogene, renders this cell line IL-3 independent and continuously growing in the presence of G-CSF, nontumorigenic and with an apparent block at the level of promyelocyte/myelocyte (32D-Ha-ras). After infection with Abelson murine leukemia virus containing a v-abl oncogene, the cell line originates (32D-abl) that is also IL-3 independent but is tumorigenic and unable to differentiate in the presence of G-CSF. This cellular model allowed us to study the relationship between distinct steps of cell differentiation, neoplastic transformation, and C3 synthesis, activation, and characteristics of binding. We demonstrated that C3 synthesis, release, and cleavage are properties already present in the progenitor 32DCl3(G) cells. The more differentiated 32D-Ha-ras cells acquired C3 acceptor sites, apparently completely saturated by the constitutively released molecules. The transformation with Abelson murine leukemia virus, although it did not affect all these properties, let the cells bind considerable amounts of C3-related fragments activated in normal murine serum through the alternative pathway. This last event was a result of the acquisition of PMSF-sensitive serine proteases associated with the plasma membrane.

Published

1993

47. Lipopolysaccharide-induced suppression of erythrocyte binding and phagocytosis via Fc gamma RI, Fc gamma RII, Fc gamma RIII, and CR3 receptors in murine macrophages.

Author

Sundaram R, O'Connor M, Cicero M, Ghaffar A, Gangemi JD, and Mayer EP

Subjects

Animals, Complement C3b metabolism, Cytokines biosynthesis, Cytokines pharmacology, Cytokines physiology, Depression, Chemical, Erythrocytes drug effects, Erythrocytes metabolism, Immunoglobulin G immunology, Kinetics, Lipopolysaccharides pharmacokinetics, Macrophages drug effects, Macrophages metabolism, Male, Mice, Mice, Inbred C3H, Phagocytosis physiology, Receptors, Complement drug effects, Receptors, Complement metabolism, Receptors, IgG drug effects, Receptors, IgG metabolism, Sheep, Complement C3 metabolism, Erythrocytes physiology, Lipopolysaccharides pharmacology, Macrophages ultrastructure, Phagocytosis drug effects, Receptors, Complement physiology, Receptors, IgG physiology

Abstract

In this study we have investigated the ability of lipopolysaccharide (LPS) to suppress binding and phagocytosis of erythrocytes via various receptors on mouse macrophages. Thioglycollate-elicited peritoneal macrophages were treated in vitro with LPS and the ability to bind and phagocytose radiolabeled sheep red blood cells was determined. We show that LPS can directly suppress phagocytosis of immunoglobulin G-opsonized and nonopsonized sheep red blood cells (SRBCs) by inflammatory macrophages. Suppression was dose dependent and was observed after 4 h of exposure. This effect lasted for at least 24 h following the removal of LPS. LPS suppressed the binding, rate, and absolute level of phagocytosis via Fc receptors. Phagocytosis via all Fc receptors (Fc gamma RI, Fc gamma RII, and Fc gamma RIII) was suppressed by LPS. Furthermore, suppression was not limited to Fc receptor-mediated phagocytosis because binding and uptake of C3bi-opsonized SRBCs to CR3 receptors was also decreased following LPS treatment. LPS did not exert its effects via the production of interleukin-1 (IL-1), IL-6, tumor necrosis factor alpha, or interferon alpha/beta, because antibodies to these cytokines did not abrogate the effect. The ability of LPS to suppress binding and phagocytosis of microorganisms may contribute to the toxic effects of LPS during gram-negative sepsis by preventing or delaying elimination of bacteria by host macrophages.

Published

1993

48. Evidence for three binding sites for C3 (hemolytically inactive), C3b and C3d on a CR2-positive Burkitt lymphoma-derived cell line (Raji).

Author

Barile G, Di Renzo L, Lipari M, Frati L, and Faggioni A

Subjects

Antibodies, Monoclonal immunology, Hemolysis, Humans, In Vitro Techniques, Macrophage-1 Antigen metabolism, Receptors, Complement 3b metabolism, Temperature, Tetradecanoylphorbol Acetate pharmacology, Tumor Cells, Cultured, Burkitt Lymphoma metabolism, Complement C3 metabolism, Complement C3b metabolism, Complement C3d metabolism, Receptors, Complement 3d metabolism

Abstract

The present investigation shows that C3 (hemolytic inactive) as well as C3b and C3d bind Raji, a CR2-positive Burkitt lymphoma-derived cell line. Pretreatment of the cells with OKB-7 inhibited the binding of C3, whereas pretreatment with HB-5 inhibited the binding of C3b. Furthermore, the cells coated either with OKB-7 or HB-5 bound high amounts of C3d. TPA-treated cells showed binding for C3b and weak binding for C3 and C3d. Taken together, the data suggest that Raji cells may express three binding sites for C3, C3b and C3d which can be differently modulated by anti-CR2 MoAbs and TPA.

Published

1993

49. Characterization of kinetics and target proteins for binding of human complement component C3 to the surface-exposed outer membrane of Chlamydia trachomatis serovar L2.

Author

Hall RT, Strugnell T, Wu X, Devine DV, and Stiver HG

Subjects

Amino Acid Sequence, Antibodies, Bacterial immunology, Antigen-Antibody Reactions, Antigens, Surface immunology, Chlamydia trachomatis classification, Complement Activation, Complement C3b metabolism, Flow Cytometry, Humans, Hydroxylamine, Hydroxylamines chemistry, In Vitro Techniques, Macromolecular Substances, Molecular Sequence Data, Protein Binding, Serotyping, Bacterial Outer Membrane Proteins metabolism, Chlamydia trachomatis immunology, Complement C3 metabolism

Abstract

In order to characterize the interaction of human complement with Chlamydia trachomatis, flow cytometry was used to quantitate binding of complement component C3 to elementary bodies of C. trachomatis serovar L2 preincubated in fresh serum in the presence or absence of human polyclonal chlamydial antibody. Isolation of each of the complement activation pathways revealed that C3 was activated most effectively by the alternative pathway. The degree of binding by the classical pathway was proportional to the concentration of antibody, but dual-pathway-mediated binding was not greater than antibody-independent alternative pathway binding. Electrophoresis and immunoblotting of detergent-extracted outer membrane protein-C3b complexes indicated that the chlamydial major outer membrane protein was the primary cell surface moiety binding C3b in both the presence and absence of specific antibody. Hydroxylamine cleavage of outer membrane protein-C3b complexes provided evidence that the majority of C3b is bound to the major outer membrane protein by hydroxyl ester bonds. This result was also unchanged by the presence of specific antibody. An unexpected finding was the apparent binding of anti-C3 antibody to a 40-kDa protein of the chlamydial outer membrane complex, perhaps indicating C3 mimicry on the part of the chlamydial major outer membrane protein.

Published

1993

50. Studies on the structure of complement C3 and the stability of C3 derived phagocytic ligands C3b/iC3b in SJL/J and BALB/c mice.

Author

Lynch DM, Kay PH, Papadimitriou JM, and Grounds MD

Subjects

Animals, Autoimmune Diseases genetics, Autoimmune Diseases immunology, Complement Activation, Complement C3 genetics, Complement C3 metabolism, Complement C3b metabolism, Female, Immunogenetics, Male, Mice, Mice, Inbred BALB C, Molecular Structure, Myositis genetics, Myositis immunology, Phagocytosis, Polymorphism, Genetic, Species Specificity, Complement C3 chemistry

Abstract

Female SJL/J mice are more susceptible to development of experimental autoimmune myositis than most other mouse strains. Since complement has been implicated in the pathogenesis of inflammatory muscle disease in humans, quantitative and qualitative studies of complement C3 were undertaken in SJL/J and BALB/c mice to determine whether complement may influence disease susceptibility in SJL/J mice. In accordance with previous studies, mature male and female BALB/c mice were shown to have similar serum C3 concentrations. However, differences were found between mature male and female SJL/J mice. Male SJL/J mice have significantly higher serum C3 concentrations than SJL/J females and both sexes of BALB/c mice suggesting that serum C3 concentration may be variably influenced by sex in some mouse strains. Qualitatively, SJL/J mice were shown to have a different allotypic form of C3 (C3F) compared to the common electrophoretically slow form (C3S) found in BALB/c mice and most other mouse strains. Furthermore, studies on the decay rate of C3 revealed that C3b/iC3b fragments are converted to C3c/d at a faster rate in sera from female SJL/J mice compared to female BALB/c mice. Because removal and solubility of immune complexes is influenced by complement C3, it is possible that the more rapid decay of the phagocytic ligands C3b/iC3b may account for the increased susceptibility to development of autoimmune disease in female SJL/J mice.

Published

1993