Your search keyword '"C4b-binding protein"' showing total 14 results

1. C4b-binding protein: The good, the bad and the deadly. Novel functions of an old friend.

Author

Ermert, David and Blom, Anna M.

Subjects

*CARRIER proteins, *PROTEIN kinase inhibitors, *BLOOD plasma, *GLYCOPROTEIN analysis, *ANTICOAGULANTS, *INFLAMMATION

Abstract

C4b-binding protein (C4BP) is best known as a potent soluble inhibitor of the classical and lectin pathways of the complement system. This large 500 kDa multimeric plasma glycoprotein is expressed mainly in the liver but also in lung and pancreas. It consists of several identical 75 kDa α-chains and often also one 40 kDa β-chain, both of which are mainly composed of complement control protein (CCP) domains. Structure-function studies revealed that one crucial binding site responsible for inhibition of complement is located to CCP1-3 of the α-chain. Binding of anticoagulant protein S to the CCP1 of the β-chain provides C4BP with the ability to strongly bind apoptotic and necrotic cells in order to prevent inflammation arising from activation of complement by these cells. Further, C4BP interacts strongly with various types of amyloid and enhances fibrillation of islet amyloid polypeptide secreted from pancreatic beta cells, which may attenuate pro-inflammatory and cytotoxic effects of this amyloid. Full deficiency of C4BP has not been identified but non-synonymous alterations in its sequence have been found in haemolytic uremic syndrome and recurrent pregnancy loss. Furthermore, C4BP is bound by several bacterial pathogens, notably Streptococcus pyogenes , which due to inhibition of complement and enhancement of bacterial adhesion to endothelial cells provides these bacteria with a survival advantage in the host. Thus, depending on the context, C4BP has a protective or detrimental role in the organism. [ABSTRACT FROM AUTHOR]

Published

2016

2. An evaluation of association between common variants in C4BPB/C4BPA genes and schizophrenia.

Author

Wang, Shuihong, Lu, Houquan, Ni, Jianliang, Zhang, Jiangtao, Tang, Wenxin, Lu, Weihong, Cai, Jun, and Zhang, Chen

Subjects

*SCHIZOPHRENIA risk factors, *CARRIER proteins, *EPIDEMIOLOGY, *PREGNANCY complications, *SINGLE nucleotide polymorphisms, *DISEASE susceptibility, *CHINESE people, *DISEASES

Abstract

Epidemiological studies have indicated that both maternal bacterial and viral infections during pregnancy increase the risk of schizophrenia among offspring, but to date there is not clear explanation for this increased risk. Previously, the decreased C4b-binding protein (C4BP), a potent circulating soluble inhibitor of the classical and lectin pathways of complement, was reported to be associated with risk of schizophrenia. Here, we analyzed 4 common single nucleotide polymorphisms (SNPs) of C4BPB and 5 SNPs of C4BPA in a group of 556 schizophrenia patients and a matched group of 610 healthy controls to see if the genes C4BPB and C4BPA, which encode C4BP, may confer a susceptibility to schizophrenia. Comparing the genotype and allele frequencies of those SNPs between cases and controls, we found no association between the C4BPB / C4BPA variants and schizophrenia. Our results provided preliminary evidence that C4BPB / C4BPA may not confer susceptibility to schizophrenia among Han Chinese. Further genetic studies from large-scale population are required to obtain more conclusive results. [ABSTRACT FROM AUTHOR]

Published

2015

3. Dysregulation of Protein S in COVID-19.

Author

Sim, Martha M.S. and Wood, Jeremy P.

Abstract

Coronavirus Disease 2019 (COVID-19) has been widely associated with increased thrombotic risk, with many different proposed mechanisms. One such mechanism is acquired deficiency of protein S (PS), a plasma protein that regulates coagulation and inflammatory processes, including complement activation and efferocytosis. Acquired PS deficiency is common in patients with severe viral infections and has been reported in multiple studies of COVID-19. This deficiency may be caused by consumption, degradation, or clearance of the protein, by decreased synthesis, or by binding of PS to other plasma proteins, which block its anticoagulant activity. Here, we review the functions of PS, the evidence of acquired PS deficiency in COVID-19 patients, the potential mechanisms of PS deficiency, and the evidence that those mechanisms may be occurring in COVID-19. [ABSTRACT FROM AUTHOR]

Published

2022

4. Complement regulator C4BP binds to Staphylococcus aureus and decreases opsonization

Author

Hair, Pamela S., Wagner, Sara M., Friederich, Patricia T., Drake, Richard R., Nyalwidhe, Julius O., and Cunnion, Kenji M.

Subjects

*CARRIER proteins, *METHICILLIN-resistant staphylococcus aureus, *COBRA venom factor, *SURGICAL site infections, *SKIN infections, *OPSONINS & opsonic index, *IMMUNE response

Abstract

Abstract: Staphylococcus aureus is the major cause of human skin and soft-tissue infections as well as invasive infections like post-operative wound infections, septic arthritis, and osteomyelitis. The complement system plays an important role in the immunological control of many bacteria, but can be inhibited by a variety of strategies including recruitment of complement regulatory proteins like C4b-binding protein (C4BP). These experiments demonstrate that S. aureus opsonization with C4b occurs rapidly in serum and is predominantly initiated by anti-staphylococcal antibodies. Much of the S. aureus-bound C4b is quickly cleaved to the inactive forms iC4b and C4d. Clinical S. aureus strains rapidly bind significant amounts of the complement regulator C4BP from serum. S. aureus also binds purified C4BP. S. aureus-bound C4BP functions as a cofactor for factor I-mediated C4b cleavage to iC4b and C4d. In the absence of factor I, C4BP decreases classical pathway-mediated deposition of C3b on the S. aureus surface by inhibiting the classical pathway C3-convertase. In summary, C4BP is recruited to the S. aureus surface where it functions to inhibit C4 complement effectors, suggesting a previously undescribed immune evasion strategy for this pathogen. [Copyright &y& Elsevier]

Published

2012

5. Complement evasion strategies of pathogens—Acquisition of inhibitors and beyond

Author

Blom, Anna M., Hallström, Teresia, and Riesbeck, Kristian

Subjects

*MONOCLONAL antibodies, *SERUM, *VITRONECTIN, *EXTRACELLULAR matrix, *CARRIER proteins, *VACCINE research, *STAPHYLOCOCCUS aureus, *COMPLEMENT (Immunology)

Abstract

Abstract: Activation of the complement system and resulting opsonisation with C3b are key events of the innate immune defense against infections. However, a wide variety of bacterial pathogens subvert complement attack by binding host complement inhibitors such as C4b-binding protein, factor H and vitronectin, which results in diminished opsonophagocytosis and killing of bacteria by lysis. Another widely used strategy is production of proteases, which can effectively degrade crucial complement components. Furthermore, bacterial pathogens such as Moraxella catarrhalis and Staphylococcus aureus capture and incapacitate the key complement component C3. The current review describes examples of these three strategies. Targeting binding sites for complement inhibitors on bacterial surfaces and complement-degrading proteases with vaccine-induced antibodies may be used to enhance a common vaccine design strategy that depends on the generation of complement-dependent bactericidal and opsonophagocytic antibody activities. [Copyright &y& Elsevier]

Published

2009

6. Native, amyloid fibrils and β-oligomers of the C-terminal domain of human prion protein display differential activation of complement and bind C1q, factor H and C4b-binding protein directly

Author

Sjöberg, Andreas P., Nyström, Sofie, Hammarström, Per, and Blom, Anna M.

Subjects

*CARRIER proteins, *PROTEIN binding, *PROTEINS, *ATP-binding cassette transporters

Abstract

Abstract: Prion protein (PrP) is an endogenous protein involved in the pathogenesis of bovine spongiform encephalopathy and Creutzfeldt–Jakob disease. Murine PrP has been reported to bind C1q and activate the classical pathway of complement in a copper-dependent manner. Here we show that various conformational isoforms (native, amyloid fibrils, and β-oligomers) of recombinant human PrP (90–231 and 121–231) bind C1q and activate complement. PrP binds both the globular head and collagenous stalk domains of C1q. Native, β-oligomeric and amyloid fibrils of PrP all activate the classical and alternative pathways of complement to different extent. However, they do not trigger the lectin pathway. Of the tested PrP conformational isoforms we find that β-oligomers bind C1q and activate complement most strongly. Membrane attack complex formation initiated by PrP is subdued in comparison to deposition of early complement components. This is most likely attributed to the interaction between human PrP and complement inhibitors factor H and C4b-binding protein. Accordingly, PrP-triggered complement activation in the terminal pathway was increased in serum lacking C4b-binding protein. Taken together the present study indicates that complement activation may be an important factor in human prion diseases, suggesting that complement induced activities may prove relevant therapeutic targets. [Copyright &y& Elsevier]

Published

2008

7. Complement regulation in human atherosclerotic coronary lesions: Immunohistochemical evidence that C4b-binding protein negatively regulates the classical complement pathway, and that C5b-9 is formed via the alternative complement pathway

Author

Oksjoki, Riina, Kovanen, Petri T., Mäyränpää, Mikko I., Laine, Petri, Blom, Anna M., Meri, Seppo, and Pentikäinen, Markku O.

Subjects

*ATHEROSCLEROTIC plaque, *CARRIER proteins, *CHROMATOGRAPHIC analysis, *GLYCOPROTEINS

Abstract

Abstract: Objective: The complement system is activated in human atherosclerotic lesions and may hence aggravate local inflammation. We studied the presence and localization of C4b-binding protein (C4bp), the major inhibitor of the classical complement pathway, in human atherosclerotic lesions in relation to complement activation products and protein S, which circulates in complex with C4bp. Methods and results: Immunohistochemistry of human coronary arteries showed C4bp to be virtually absent in normal arteries but present in early and advanced atherosclerotic lesions. In the lesions, C4bp is associated with proteoglycans, and affinity chromatography showed that C4bp interacts with human arterial proteoglycans. Areas containing C4bp also contained IgM and C4 suggesting that C4bp is involved in the regulation of the classical complement pathway. However, C5b-9 was virtually absent in these areas but, instead, colocalized with properdin deeper in the intima, suggesting that C5b-9 is formed by the alternative complement pathway. A fraction of C4bp was associated with protein S and apoptotic cells. Conclusions: The results indicate that C4bp regulates the classical complement pathway in human atherosclerotic lesions. Thus, unlike the alternative pathway, the classical complement pathway does not generate C5b-9, but is likely to be involved in the clean-up of apoptotic cells and cell debris in the arterial intima. [Copyright &y& Elsevier]

Published

2007

8. Role of the C3b-binding site on C4b-binding protein in regulating classical pathway C5 convertase

Author

Rawal, Nenoo and Pangburn, Michael K.

Subjects

*ERYTHROCYTES, *BLOOD cells, *CELLS, *BLOOD cell count

Abstract

Abstract: A high affinity C5 convertase is generated when a C3 convertase deposits additional C3b molecules on and around itself thereby switching the substrate specificity of C3 convertase from C3 to C5. In the present study the role of the additional C3b molecules in influencing the regulation of classical pathway C5 convertase by C4b-binding protein (C4BP) was examined and compared to its precursor, the C3 convertase. Determination of IC50 for inhibiting formation of the high affinity C5 convertase and for enhancing its decay (72 and 20nM) were found to be similar to those obtained for the surface-bound C3 convertase (35 and 11nM). No difference was observed in the cofactor activity of C4BP for surface-bound C4b alone or when in complex with C3b. Analysis of binding interactions between C4BP and EAC1,C4b cells revealed an average apparent dissociation constant (12nM) similar to that obtained with EAC1,C4b cells with C3b on them (11nM). Increasing the C4b or C3b density on the cell surface did not alter the affinity of C4BP. The data suggest that C4BP regulates the C5 convertase by mechanisms similar to those observed for the C3 convertase. Since the IC50 for inhibiting formation of the soluble C3 convertase (5nM) is 50–80-fold below the normal serum concentration of C4BP (250–400nM), C4BP in blood effectively prevents formation of classical pathway C3 convertase in the fluid phase. Although deposition of additional C3b molecules is necessary to convert a C3 convertase to a high affinity C5 convertase, the additional C3b molecules play no role in the regulation of C5 convertase by C4BP. [Copyright &y& Elsevier]

Published

2007

9. Protein S in cancer patients with non-metastatic solid tumours.

Author

Battistelli, S., Vittoria, A., Cappelli, R., Stefanoni, M., and Roviello, F.

Subjects

PROTEIN S, CIRCULATING anticoagulants, ACUTE phase reaction, FIBRINOGEN, TUMORS

Abstract

Abstract: Aims: To study protein S, as an acute phase protein, for its relationships with C4b-BP (C4BP), fibrinogen and Factor VIII:C in a group of patients with solid tumours, without proven metastases. Methods: Eighty-one consecutive patients with gastrointestinal or pelvic adenocarcinoma (TNM staging: T1-3, N0-2, M0) and 58 healthy subjects were evaluated for plasma free and total protein S antigen, protein S activity, C4BP, fibrinogen and Factor VIII:C. Results: When compared to the control group, the total protein S, the C4BP, the fibrinogen and the Factor VIII:C mean levels were significantly higher in the cancer group, but there was no significant difference for the free and the functional protein S mean concentrations. In both groups the free protein S was correlated with the functional and the total protein S; moreover the latter was significantly correlated with the C4BP, whereas it was significantly correlated with the fibrinogen and the Factor VIII:C only in the cancer group. In addition, a high correlation was found among the C4BP, the fibrinogen and the Factor VIII:C. Conclusions: Our data show that in these patients there is an acute phase response and suggest that, in the thrombophilic early cancer screening, determination of free protein S is redundant. [Copyright &y& Elsevier]

Published

2005

10. Complement inhibitor C4b-binding protein—friend or foe in the innate immune system?

Author

Blom, Anna M., Villoutreix, Bruno O., and Dahlbäck, Björn

Subjects

*DRUG receptors, *IMMUNE system, *ISOPENTENOIDS, *B cells

Abstract

The complement system constitutes an important component of the defence against foreign organisms, functioning both in innate and adaptive immune systems. It is potentially harmful also to the own organism and is therefore tightly regulated by a number of membrane-bound and soluble factors. C4b-binding protein (C4BP) is a potent circulating soluble inhibitor of the classical and lectin pathways of complement. In recent years, the relationships between the structure of C4BP and its functions have been elucidated using a combination of computer-based molecular analysis and recombinant DNA technologies. Moreover, two novel functions have recently been ascribed to C4BP. One is the ability of C4BP to localize complement regulatory activity to the surface of apoptotic cells via its interaction with the membrane-binding vitamin K-dependent protein S. The other is the ability of C4BP to act as a survival factor for B cells due to an interaction with CD40. The complement regulatory activity of C4BP is not only beneficial because it is also explored by pathogens such as Neisseria gonorrhoeae, Bordetella pertussis, Streptococcus pyogenes, Escherichia coli K1, and Candida albicans, that bind C4BP to their surfaces. This contributes to the serum resistance and the pathogenicity of these bacteria. In this review, the structural requirements and functional importance of the interactions between C4BP and its various ligands are discussed. [Copyright &y& Elsevier]

Published

2004

11. CCP1–4 of the C4b-binding protein α-chain are required for factor I mediated cleavage of complement factor C3b

Author

Blom, Anna M., Kask, Lena, and Dahlbäck, Björn

Subjects

*CARRIER proteins, *FIBRINOGEN, *ALANINE

Abstract

C4b-binding protein (C4BP) is a potent regulator of the complement system because it strongly inhibits the classical pathway of complement. Furthermore, C4BP serves as a cofactor to factor I (FI) in the cleavage of fluid phase C3b and can, therefore, influence the alternative pathway of complement. The major form of C4BP in plasma consists of seven identical α-chains and one β-chain. Both types of subunits are composed of complement control protein (CCP) domains, eight such domains make up one α-chain. To elucidate the structural requirements for the interaction between C3b and the α-chain, nineteen recombinant C4BP variants were used: six truncated monomeric variants, nine polymeric variants in which individual CCPs were deleted, and finally four variants in which double alanine residues were introduced between CCPs. We found that C4BP requires all four N-terminal CCPs of the α-chain, with CCP2 and 3 being the most important, to act as a cofactor in the cleavage of C3b. Also, a cluster of positively charged amino acids on the interface between CCP1 and 2 is involved in the binding. Compared to the interaction with C4b, we conclude that binding of C3b to C4BP requires larger molecular surface on C4BP. We found that C4BP was able to act as cofactor in degradation of surface bound C3b and to accelerate decay of alternative C3-convertase. However, in both cases 1000-fold molar excess of C4BP over factor H (FH), well known inhibitor of the alternative pathway, was required to obtain the same effect. [Copyright &y& Elsevier]

Published

2003

12. Contribution of interactions between complement inhibitor C4b-binding protein and pathogens to their ability to establish infection with particular emphasis on Neisseria gonorrhoeae

Author

Blom, Anna M. and Ram, Sanjay

Subjects

*COMPLEMENT inhibition, *CARRIER proteins, *NEISSERIA infections, *NEISSERIA gonorrhoeae, *NATURAL immunity, *HOST-bacteria relationships, *COMPLEMENT activation, *MONOCLONAL antibodies

Abstract

Abstract: Complement activation and resulting opsonisation with C3b form key arms of the innate immune defense against infections. However, a wide variety of pathogens subvert complement attack by binding host complement inhibitors, which results in diminished opsonophagocytosis and killing of bacteria by lysis. Human C4b-binding protein (C4BP) binds Neisseria gonorrhoeae and Streptococcus pyogenes, both uniquely human pathogens. This binding specificity is circumvented by other bacterial species, which bind C4BP from numerous mammalian hosts that they infect. Binding of C4BP to Neisseria is mediated by outer membrane porin proteins and appears to be one of the main factors mediating serum resistance. Targeting C4BP binding sites on bacterial surfaces with vaccine-induced antibodies may block binding of C4BP and enhance a common vaccine design strategy that depends on the generation of complement-dependent bactericidal and opsonophagocytic antibody activities. [Copyright &y& Elsevier]

Published

2008

13. Binding of complement regulatory proteins to Group A Streptococcus

Author

Oliver, Maria A., Rojo, José M., Rodríguez de Córdoba, Santiago, and Alberti, Sebastián

Subjects

*PROTEIN binding, *COMPLEMENT (Immunology), *CARRIER proteins, *STREPTOCOCCUS, *STREPTOCOCCAL diseases, *NATURAL immunity, *IMMUNE system, *IMMUNOLOGY

Abstract

Abstract: Streptococcus pyogenes or Group A Streptococcus (GAS) is the etiologic agent of important human infections such as acute pharyngitis, impetigo, rheumatic fever and the streptococcal toxic shock syndrome. Binding of the complement regulatory proteins factor H, factor H-like protein 1 (FHL-1), C4b-binding protein (C4BP), or CD46 is a crucial step in the pathogenesis of these infections. M protein is the GAS protein that generally mediates these interactions. However, a detailed analysis of the reports that have investigated the binding of complement regulatory components to GAS indicates that this microorganism has evolved alternative mechanisms for the recruitment of complement regulatory proteins to the bacterial surface. This article summarizes these data to provide a starting point for future research aimed at the characterization of additional mechanisms developed by GAS to evade the immune system. [Copyright &y& Elsevier]

Published

2008

14. Host–pathogen interactions in Streptococcus pyogenes infections, with special reference to puerperal fever and a comment on vaccine development

Author

Areschoug, Thomas, Carlsson, Fredric, Stålhammar-Carlemalm, Margaretha, and Lindahl, Gunnar

Subjects

*STREPTOCOCCUS pyogenes, *PUERPERAL septicemia, *CARRIER proteins, *IMMUNE system

Abstract

Abstract: Streptococcus pyogenes (group A streptococcus) causes a variety of diseases, including acute pharyngitis, impetigo, rheumatic fever and the streptococcal toxic shock syndrome. Moreover, S. pyogenes was responsible for the classical example of a nosocomial infection, the epidemics of puerperal fever (childbed fever) that caused the death of numerous women in earlier centuries. The most extensively studied virulence factor of S. pyogenes is the surface M protein, which inhibits phagocytosis and shows antigenic variation. Recent data indicate that many M proteins confer phagocytosis resistance because the variable N-terminal region has non-overlapping sites that specifically bind two components of the human immune system, the complement inhibitor C4b-binding protein (C4BP) and IgA-Fc. Concerning puerperal fever, molecular and epidemiological analysis suggests that the S. pyogenes surface protein R28 may have played a pathogenetic role in these epidemics. This article summarizes the properties of M protein and the R28 protein and considers a potential problem encountered in connection with the use of animal models for vaccine development. [Copyright &y& Elsevier]

Published

2004