C4b-Binding Protein, a Regulatory Component of the Classical Pathway of Complement, Is an Acute-Phase Protein and Is Elevated in Systemic Lupus Erythematosus

Barnum, Scott R.; Dahlbäck, Björn

doi:10.1159/000463131

Cited by 62 publications

(31 citation statements)

References 27 publications

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“…In previous studies it has been established that C4BP is an acute-phase reactant that increases its plasma concentration 2-to 4-fold [8][9][10]. Conforming to these data, the evolu tion of the C4BP levels in the serial samples from patients who have undergone orthoped ic surgery shows an elevation of the concen tration of total C4BP during the postsurgical acute-phase response ( fig.…”

Section: Evolution O F the C4bp Isoform Pattern After Orthopedic Surgerymentioning

confidence: 75%

“…These two activities are performed by two distinct polypeptides of 70 and 45 kDa known as a-and (3-chains, respectively [5], C4BP is present in plasma in various isoforms with different a/(3-composition, a7:(31 (nor mally the major isoform), a7:(30 and a6:|31 [7], C4BP is described as an acute-phase reactant that elevates its concentration in plasma 2-to 4-fold in the acute-phase response [8][9][10], When C4BP is induced, the expression of the C4BPA and C4BPB genes is differentially modulated [11,12], determining changes in the proportion of the C4BP isoforms. Ele vated concentrations of C4BP(3-containing isoforms may result in a lack of free protein S and in an inactivation of the protein C anticoagulatory pathway [13][14][15][16][17][18].…”

Section: Introductionmentioning

confidence: 99%

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Modulation of C4b-Binding Protein Isoforms during the Acute Phase Response Caused by Orthopedic Surgery

Criado‐García

González-Rubio²,

López‐Trascasa³

et al. 1997

Pathophysiol Haemos Thromb

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Orthopedic surgery is described as an event with a high risk of thromboembolic diseases. This is probably a consequence of a synergistic combination of different risk factors in the patients subjected to this type of surgery, including age, immobilization, anesthesia and different hypercoagulable states. After surgery patients develop an acute-phase response that leads to changes in several plasma proteins. One of these proteins is the complement regulator C4b-binding protein (C4BP). We have recently shown that in some acute-phase patients C4BP is incorrectly controlled (with elevation of the C4BPΒ-containing isoforms), leading to a potential hypercoagulable state by decreasing the plasma levels of free (active) protein S. Here we have studied whether patients subjected to orthopedic surgery have an appropriate modulation of the C4BP isoforms during their postoperative acute-phase responses. We have analyzed the evolution of the C4BP isoforms in serial samples from 11 patients who have undergone knee (or hip) prosthesis surgery (mean age 70 years), or scoliosis surgery (mean age 18 years). Our data suggest a similar evolution of C4BP isoforms in all these patients, with an almost exclusive increase of C4BP isoforms lacking C4BPΒ polypeptides and steady levels of free protein S.

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Section: Evolution O F the C4bp Isoform Pattern After Orthopedic Surgerymentioning

confidence: 75%

Section: Introductionmentioning

confidence: 99%

Modulation of C4b-Binding Protein Isoforms during the Acute Phase Response Caused by Orthopedic Surgery

Criado‐García

González-Rubio²,

López‐Trascasa³

et al. 1997

Pathophysiol Haemos Thromb

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“…C4BP also acts as a cofactor to serine protease factor I in the degradation and inactivation of C4b (11) and C3b (12). C4BP is an acute phase protein (13), but only the ␣7␤0 form increases in expression during inflammation (14), ensuring that PS (the ␤-chain ligand) will not be depleted from plasma, which could otherwise lead to severe thrombotic disorders. 1 The abbreviations used are: MBL, mannose binding lectin; CR, complement receptor; C4BP, C4b-binding protein; CCP, complement control protein; HBSS, Hanks' balanced salt solution; PE, phycoerythrin; PS, protein S; EGF, epidermal growth factor; SHBG, sex hormone binding globulin; PBS, phosphate-buffered saline; CFSE, 5-(and 6-)carboxyfluorescein diacetate succinimidyl ester; mAb, monoclonal antibody; ELISA, enzyme-linked immunosorbent assay; SLE, systemic lupus erythematosus.…”

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confidence: 99%

The C4b-binding Protein-Protein S Complex Inhibits the Phagocytosis of Apoptotic Cells

Kask

Trouw²,

Dahlbäck

et al. 2004

Journal of Biological Chemistry

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The phagocytosis of apoptotic cells is a complex process involving numerous interactions between the target cell and the macrophage. We have examined a role of the major soluble inhibitor of the classic and lectin complement pathways, C4b-binding protein (C4BP), in the clearance of apoptotic cells. The major form of C4BP present in blood is composed of seven ␣-chains and one ␤-chain, which binds protein S (PS). Approximately 70% of all PS in human plasma is trapped in such a complex and is able to localize C4BP to the surface of apoptotic cells due to the high affinity to phosphatidylserine. Free PS has recently been shown to enhance phagocytosis of apoptotic cells by macrophages. We observed a stimulatory effect of free PS on the engulfment of apoptotic cells (BL-41 and Jurkat) by primary human macrophages or THP-1 cells and a decrease of activity in serum depleted of PS in agreement with previous results. However, we also show that the process is strongly inhibited in the presence of the C4BP-PS complex. Addition of the C4BP-PS complex to serum deficient in both molecules abolished the enhancing effect of serum on phagocytosis. The effect of both free PS and the C4BP-PS complex could be inhibited with monoclonal antibody directed against the Gla domain of PS. Although the presence of the C4BP-PS complex on apoptotic cells may lead to decreased phagocytosis, it may still be beneficial to the host, since it could prevent secondary necrosis because it inhibits further complement attack.

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“…The average plasma concentration of C4BP is ϳ260 nM (150 g/ml) (10), although its levels may increase up to 4-fold during inflammation, infection, or tissue damage (11,12). Plasma levels represent a balance between C4BP production and removal.…”

Section: C4b-binding Protein (C4bp)mentioning

confidence: 99%

“…In addition, the ␣-chains have been found to contain binding sites for bacterial surface proteins from Streptococcus pyogenes (7) and heparin (8). The heparin interactive site, which overlaps with the C4b interactive site, encompasses a cluster of positively charged amino acids involving Arg residues at positions 39, 64, and 66 (9).The average plasma concentration of C4BP is ϳ260 nM (150 g/ml) (10), although its levels may increase up to 4-fold during inflammation, infection, or tissue damage (11,12). Plasma levels represent a balance between C4BP production and removal.…”

mentioning

confidence: 99%

The α-Chains of C4b-binding Protein Mediate Complex Formation with Low Density Lipoprotein Receptor-related Protein

Westein¹,

Denis²,

Bouma³

et al. 2002

Journal of Biological Chemistry

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C4b-binding protein (C4BP) is a heparin-binding protein that participates in both the complement and hemostatic system. We investigated the interaction between C4BP and low density lipoprotein receptorrelated protein (LRP), an endocytic receptor involved in the catabolism of various heparin-binding proteins. Both plasma-derived C4BP and recombinant C4BP consisting of only its ␣-chains (rC4BP␣) bound efficiently to immobilized LRP, as determined by surface plasmon resonance analysis. Complementary, two distinct fragments of LRP, i.e. clusters II and IV, both associated to immobilized rC4BP␣, and binding could be inhibited by the LRP antagonist receptor-associated protein. Further analysis showed that association of rC4BP␣ to LRP was inhibited by heparin or by anti-C4BP antibody RU-3B9, which recognizes the heparinbinding region of the C4BP ␣-chains. In cellular degradation experiments, LRP-expressing fibroblasts effectively degraded 125 I-labeled rC4BP␣, whereas their LRP-deficient counterparts displayed a 4-fold diminished capacity of degrading 125 I-rC4BP␣. Finally, initial clearance of C4BP in mice was significantly delayed upon co-injection with receptor-associated protein. In conclusion, our data demonstrate that the ␣-chains of C4BP comprise a binding site for LRP. We propose that LRP mediates at least in part the catabolism of C4BP and, as such, may regulate C4BP participation in complement and hemostatic processes. C4b-binding protein (C4BP)1 is a plasma protein, which serves as a regulator of the complement system (1). C4BP binds the complement protein C4b, which results in enhancement of factor I-mediated degradation of C4b and inhibition of the classical pathway C3 convertase (C4b2a) complex (1). In plasma, C4BP may serve as a carrier protein for at least two other plasma proteins: the vitamin K-dependent anticoagulant Protein S and serum amyloid P component (1). In addition, C4BP may interact with coagulation factor VIII as well (2). The majority of the C4BP molecules (ϳ80%) consist of seven identical ␣-chains and a unique ␤-chain, whereas other isoforms lack either one of the ␣-chains or the ␤-chain (3). The ␤-chain is involved in the interaction with Protein S (4), and complex formation with serum amyloid P component (SAP) and complement proteins is mediated by the ␣-chains (5, 6). In addition, the ␣-chains have been found to contain binding sites for bacterial surface proteins from Streptococcus pyogenes (7) and heparin (8). The heparin interactive site, which overlaps with the C4b interactive site, encompasses a cluster of positively charged amino acids involving Arg residues at positions 39, 64, and 66 (9).The average plasma concentration of C4BP is ϳ260 nM (150 g/ml) (10), although its levels may increase up to 4-fold during inflammation, infection, or tissue damage (11,12). Plasma levels represent a balance between C4BP production and removal. At present, little is known concerning the molecular mechanisms that control the removal of C4BP from the circulation. The notion that C4BP is able to in...

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C4b-Binding Protein, a Regulatory Component of the Classical Pathway of Complement, Is an Acute-Phase Protein and Is Elevated in Systemic Lupus Erythematosus

Cited by 62 publications

References 27 publications

Modulation of C4b-Binding Protein Isoforms during the Acute Phase Response Caused by Orthopedic Surgery

Modulation of C4b-Binding Protein Isoforms during the Acute Phase Response Caused by Orthopedic Surgery

The C4b-binding Protein-Protein S Complex Inhibits the Phagocytosis of Apoptotic Cells

The α-Chains of C4b-binding Protein Mediate Complex Formation with Low Density Lipoprotein Receptor-related Protein

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