Your search keyword '"Ghebrehiwet B"' showing total 302 results

151. Classical pathway complement activation on human endothelial cells.

Author

Yin W, Ghebrehiwet B, Weksler B, and Peerschke EI

Subjects

Animals, Carrier Proteins immunology, Cells, Cultured, Endothelial Cells cytology, Flow Cytometry, Humans, Mitochondrial Proteins immunology, Rats, Stress, Mechanical, Complement Pathway, Classical immunology, Endothelial Cells immunology, Endothelium, Vascular cytology, Endothelium, Vascular immunology

Abstract

Endothelial cells regulate vascular integrity and express complement binding proteins including gC1qR/p33 (gC1qR), which recognize C1q, a subunit of the first component of the classical complement pathway. Experiments were performed to investigate classical complement pathway activation on resting endothelial cells and endothelial cells exposed to shear stress. C1q deposition and C4 activation (C4d) were demonstrated by solid phase ELISA and flow cytometry on human microvascular and umbilical vein endothelial cells after exposure to serum or plasma. C4d deposition was accompanied by downstream complement activation including C3b and C5b-9 deposition. C4 activation failed to occur in C1q depleted serum, but was not affected by Factor B depleted serum, confirming classical complement pathway activation. Moreover, C4 activation occurred following exposure of endothelial cells to purified C1 and C4, in the absence of other plasma proteins, and in the absence of detectable cell surface IgG and IgM. Shear stress (18 dynes/cm2) increased C1q (n=9, p<0.05) and C4d (n=9, p<0.05) deposition approximately two-fold, and enhanced endothelial cell gC1qR expression (n=7, p<0.05). Treatment of endothelial cells with anti gC1qR monoclonal antibody F(ab')2 fragments reduced C4d deposition by approximately 20% (n=5, p<0.05). These data demonstrate direct classical complement pathway activation on endothelial cells. gC1qR appears to play a minor but definable role, whereas cell surface IgG or IgM are not required.

Published

2007

152. The exosporium of B. cereus contains a binding site for gC1qR/p33: implication in spore attachment and/or entry.

Author

Ghebrehiwet B, Tantral L, Titmus MA, Panessa-Warren BJ, Tortora GT, Wong SS, and Warren JB

Subjects

Animals, Antibodies, Monoclonal metabolism, Bacillus cereus metabolism, Bacillus cereus pathogenicity, Binding Sites, Caco-2 Cells, Calcium metabolism, Chelating Agents metabolism, Edetic Acid metabolism, Epithelial Cells metabolism, Epithelial Cells ultrastructure, Humans, Microscopy, Electron, Monocytes cytology, Monocytes metabolism, Nanotubes, Carbon, Neutrophils cytology, Neutrophils metabolism, Phagocytosis, Temperature, Bacillus cereus cytology, Carrier Proteins metabolism, Mitochondrial Proteins metabolism, Spores, Bacterial metabolism

Abstract

B. cereus, is a member of a genus of aerobic, gram-positive, spore-forming rod-like bacilli, which includes the deadly, B. anthracis. Preliminary experiments have shown that gC1qR binds to B. cereus spores that have been attached to microtiter plates. The present studies were therefore undertaken, to examine if cell surface gC1qR plays a role in B. cereus spore attachment and/or entry. Monolayers of human colon carcinoma (Caco-2) and lung cells were grown to confluency on 6 mm coverslips in shell vials with gentle swirling in a shaker incubator. Then, 2 microl of a suspension of strain SB460 B. cereus spores (3x10(8)/ml, in sterile water), were added and incubated (1-4 h; 36 degrees C) in the presence or absence of anti-gC1qR mAb-carbon nanoloops. Examination of these cells by EM revealed that: (1) When B. cereus endospores contacted the apical Caco-2 cell surface, or lung cells, gC1qR was simultaneously detectable, indicating upregulation of the molecule. (2) In areas showing spore contact with the cell surface, gC1qR expression was often adjacent to the spores in association with microvilli (Caco-2 cells) or cytoskeletal projections (lung cells). (3) Furthermore, the exosporia of the activated and germinating spores were often decorated with mAb-nanoloops. These observations were further corroborated by experiments in which B.cereus spores were readily taken up by monocytes and neutrophils, and this uptake was partially inhibited by mAb 60.11, which recognizes the C1q binding site on gC1qR. Taken together, the data suggest a role, for gC1qR at least in the initial stages of spore attachment and/or entry.

Published

2007

153. The contribution of gC1qR/p33 in infection and inflammation.

Author

Peerschke EI and Ghebrehiwet B

Subjects

Animals, Antigens, Bacterial immunology, Bradykinin biosynthesis, Complement System Proteins metabolism, Humans, Infections immunology, Inflammation immunology, Inflammation metabolism, Infections metabolism, Membrane Glycoproteins metabolism, Receptors, Complement metabolism

Abstract

Human gC1qR/p33 is a multi-compartmental and multi-functional cellular protein expressed on a wide range of tissues and cell types including lymphocytes, endothelial cells, dendritic cells, and platelets. Although originally isolated as a receptor for C1q by virtue of its affinity (K(d)=15-50 nM), and specificity for the globular heads of this molecule, a large body of evidence has now been accumulated which shows that in addition to C1q, gC1qR can serve as a receptor for diverse proinflammatory ligands including proteins of the plasma kinin-forming system, most notably high molecular weight kininogen (HK; K(d)=9 nM). In addition, gC1qR has been reported to recognize and bind a number of functional antigens of viral and bacterial origin. It is its ability to interact with microbial antigens and its potential to serve as a cellular protein for bacterial attachment and/or entry that has been the focus of our laboratory in the past few years. On the surface of activated platelets, gC1qR has been shown to serve as a binding site for Staphylococcus aureus and this binding is mediated by protein A. Since the binding of S. aureus to platelets is postulated to play a major role in the pathogenesis of endocarditis, gC1qR may provide a suitable surface for the initial adhesion of the bacterium. Recent data also demonstrate that the exosporium of Bacillus cereus, a member of a genus of aerobic, Gram-positive, spore-forming rod-like bacilli, which includes the deadly Bacillus anthracis, contains a binding site for gC1qR. Therefore, by virtue of its ability to recognize plasma proteins such as C1q and HK, as well as bacterial and viral antigens, cell-surface gC1qR not only is able to generate proinflammatory byproducts from the complement and kinin/kallikrein systems, but also can be an efficient vehicle and platform for a plethora of pathogenic microorganisms.

Published

2007

154. High-molecular-weight kininogen fragments stimulate the secretion of cytokines and chemokines through uPAR, Mac-1, and gC1qR in monocytes.

Author

Khan MM, Bradford HN, Isordia-Salas I, Liu Y, Wu Y, Espinola RG, Ghebrehiwet B, and Colman RW

Subjects

Antibodies, Monoclonal pharmacology, CD11a Antigen immunology, Humans, Interleukin-1 antagonists & inhibitors, Interleukin-1 genetics, Interleukin-1 metabolism, Kininogen, High-Molecular-Weight immunology, Kininogen, High-Molecular-Weight metabolism, Macrophage-1 Antigen immunology, Membrane Glycoproteins immunology, Mitogen-Activated Protein Kinases physiology, NF-kappa B physiology, Osmolar Concentration, Peptide Fragments immunology, Peptide Fragments metabolism, Peptide Fragments pharmacology, RNA, Messenger metabolism, Receptors, Cell Surface immunology, Receptors, Complement immunology, Receptors, Urokinase Plasminogen Activator, Time Factors, Chemokines metabolism, Cytokines metabolism, Kininogen, High-Molecular-Weight pharmacology, Macrophage-1 Antigen metabolism, Membrane Glycoproteins metabolism, Monocytes metabolism, Receptors, Cell Surface metabolism, Receptors, Complement metabolism

Abstract

Objective: Plasma high-molecular-weight kininogen (HK) is cleaved in inflammatory diseases by kallikrein to HKa with release of bradykinin (BK). We postulated a direct link between HKa and cytokine/chemokine release., Methods and Results: HKa, but not BK, releases cytokines tumor necrosis factor (TNF)-alpha, interleukin (IL)-1beta, IL-6, and chemokines IL-8 and MCP-1 from isolated human mononuclear cells. At a concentration of 600 nM, glutathione-S-transferase (GST) fusion proteins of kininogen domain 3 (D3), a fragment of domain 3, E7P (aaG255-Q292), HK domain 5 (D5), the D5 recombinant peptides HG (aa K420-D474) and HGK (aa H475-S626) stimulated secretion of IL-1beta from mononuclear cells. Monoclonal antibodies (MAbs) specific for D5 or specific for D3 blocked release of IL-1beta by HKa, supporting the importance of both domains. Antibodies to HK receptors on leukocytes including Mac-1, LFA-1, uPAR, and C1qR inhibited IL-1beta secretion induced by tKa 98%, 89%, 85%, and 62%, respectively. Fractionation of mononuclear cells identified the responsible cell, a blood monocyte. Inhibitors of signaling pathways NFkB, JNK, and p38 but not extracellular signal-regulated kinase (ERK) decreased cytokine release from mononuclear cells. HKa increased the synthesis of IL-1beta as deduced by an increase of IL-1beta mRNA at 1 to 2 hours., Conclusions: HKa domains 3 and 5 may contribute to the pathogenesis of inflammatory diseases by releasing IL-1beta from human monocytes using intracellular signaling pathways initiated by uPAR, beta2 integrins and gC1qR.

Published

2006

155. gC1qR/p33 blockade reduces Staphylococcus aureus colonization of target tissues in an animal model of infective endocarditis.

Author

Peerschke EI, Bayer AS, Ghebrehiwet B, and Xiong YQ

Subjects

Animals, Antibodies, Monoclonal immunology, Aortic Valve microbiology, Bacterial Adhesion, Complement C1q, Humans, Kidney microbiology, Membrane Glycoproteins immunology, Membrane Glycoproteins metabolism, Rats, Receptors, Complement immunology, Receptors, Complement metabolism, Spleen microbiology, Staphylococcal Infections microbiology, Staphylococcus aureus metabolism, Virulence, Disease Models, Animal, Endocarditis, Bacterial microbiology, Fibrinogen metabolism, Membrane Glycoproteins antagonists & inhibitors, Receptors, Complement antagonists & inhibitors, Staphylococcus aureus growth & development, Staphylococcus aureus pathogenicity

Abstract

gC1qR/p33 (gC1qR) is a ubiquitously expressed cellular protein that is also found in plasma and the extracellular matrix. In addition to its role in modulating the activation of complement and kinin cascades, gC1qR has been identified as a putative host ligand for endovascular pathogens, including Staphylococcus aureus. The present study provides evidence of the ability of soluble gC1qR to enhance S. aureus-fibrinogen interactions via simultaneously binding fibrinogen and S. aureus. This interaction was inhibited in vitro by two monoclonal antibodies (MAbs 74.5.2 and 60.11) recognizing distinct structural and functional domains of gC1qR. To evaluate the in vivo role of gC1qR, MAbs 74.5.2 and 60.11 were used in an experimental rat model of S. aureus endocarditis. Each MAb (100 mg/kg of body weight, given intraperitoneally) reached sustained (>60 h) and high (100 to 200 microg/ml) serum levels. Prophylaxis with MAb 60.11 or 74.5.2 caused substantial reductions in S. aureus colonization of aortic valves, kidneys, and the spleen compared to untreated controls. However, only MAb 74.5.2 prophylaxis therapy reached statistical significance, and only sera from animals protected with MAb 74.5.2 inhibited gC1qR-mediated S. aureus interactions with fibrinogen. Although not statistically significant, the reductions in bacterial colonization achieved with MAb 60.11 alone and in combination with MAb 74.5.2 (versus MAb 74.5.2 alone) suggest that there are effects of gC1qR blockade on S. aureus infective endocarditis in addition to blocking gC1qR-mediated S. aureus binding to fibrinogen. Such impacts may include direct modulation of complement (MAb 60.11) and kinin cascades (MAb 74.5.2) and/or activation of immune and inflammatory responses via localized immune complex formation.

Published

2006

156. Chemotaxis of human monocyte-derived dendritic cells to complement component C1q is mediated by the receptors gC1qR and cC1qR.

Author

Vegh Z, Kew RR, Gruber BL, and Ghebrehiwet B

Subjects

Animals, Antibodies pharmacology, Calreticulin antagonists & inhibitors, Carrier Proteins antagonists & inhibitors, Cell Differentiation, Cell Membrane immunology, Chemotactic Factors metabolism, Chemotactic Factors pharmacology, Chemotaxis drug effects, Complement C1q pharmacology, Dendritic Cells cytology, Dendritic Cells drug effects, Humans, In Vitro Techniques, Membrane Glycoproteins antagonists & inhibitors, Mitochondrial Proteins antagonists & inhibitors, Monocytes cytology, Monocytes immunology, Phenotype, Rabbits, Receptors, Complement antagonists & inhibitors, Calreticulin metabolism, Carrier Proteins metabolism, Chemotaxis immunology, Complement C1q metabolism, Dendritic Cells immunology, Membrane Glycoproteins metabolism, Mitochondrial Proteins metabolism, Receptors, Complement metabolism

Abstract

Dendritic cells (DCs) are recruited to inflammatory sites where they phagocytose and process antigens for subsequent presentation to the T lymphocytes in the lymphoid tissue. Several leukocyte chemoattractants and their specific receptors have been shown to induce the migration of DC. The complement protein C1q has multiple immune functions including acting as a chemoattractant for neutrophils, eosinophils and mast cells. Therefore, the objective of this study was to determine if soluble C1q can induce chemotaxis of DC. Culturing cells in GM-CSF and IL-4 for 5 to 7 days generated human monocyte-derived DCs. In addition, LPS was added from day 5 to 7 to induce DC maturation. Cells were classified as either immature or mature DC by assessing the cell surface markers by flow cytometry, phagocytosis of dextran-FITC and T cell proliferation in an allogenic MLR. Immature DCs express the C1q receptors (C1qR), gC1qR and cC1qR/CR and, accordingly, display a vigorous migratory response to soluble C1q with maximal cell movement observed at 10-50nM. In contrast, mature DCs neither express C1qR nor do move to a gradient of soluble C1q. Varying the concentration gradient of C1q (checkerboard assay) showed that the protein largely induces a chemotactic response. Finally, blocking gC1qR and cC1qR/CR by using specific antibodies abolished the chemotactic response to C1q but had no effect on a different chemoattractant C5a. These results clearly demonstrate that C1q functions as a chemotactic factor for immature DC, and migration is mediated through ligation of both gC1qR and cC1qR/CR.

Published

2006

157. gC1qR/p33 serves as a molecular bridge between the complement and contact activation systems and is an important catalyst in inflammation.

Author

Ghebrehiwet B, CebadaMora C, Tantral L, Jesty J, and Peerschke EI

Subjects

Carrier Proteins genetics, Hemolysis, Humans, Mitochondrial Proteins genetics, Recombinant Fusion Proteins genetics, Recombinant Fusion Proteins immunology, Carrier Proteins immunology, Complement Activation physiology, Complement C1q immunology, Inflammation immunology, Mitochondrial Proteins immunology

Abstract

The receptor for the globular heads of C1q, gC1qR/p33, is a ubiquitously expressed protein, which is distributed both intracellularly and on the cell-surface protein. In addition to C1q, this molecule also is able to bind several other biologically important plasma ligands, including high-molecular-weight kininogen (HK), factor XII (FXII), and multimeric vitronectin. Previous studies have shown that incubation of FXII, prekallikrein, and HK with gC1qR leads to a zinc-dependent and FXII-dependent conversion of prekallikrein to kallikrein, a requisite for kinin generation. In addition, these studies showed that normal plasma, but not plasma deficient in FXII, PK, or HK, activate upon binding to endothelial cells (EC), and that this activation could be inhibited by antibody to gClqR. In these studies, we show that incubation of serum with microtiter plate bound gC1qR results in complement activation, as evidenced by the binding and activation of C1 and generation of C4d. However, neither Clq-deficient serum nor a truncated form of gC1qR (gC1qRA74-96), supported complement activation. Taken together, the data strongly suggest that at sites of inflammation, such as vasculitis and atherosclerosis, where gC1qR as well as its two important plasma ligands, C1q and HK, have been shown to be simultaneously present, soluble or cell-surface-expressed gC1qR may contribute to the inflammatory process by modulating complement activation, kinin generation, and perhaps even initiation of clotting via the contact system. Based on these and other published data, we propose a model of inflammation in which atherogenic factors (e.g., immune complexes, virus, or bacteria) are perceived not only to convert the endothelium into a procoagulant and proinflammatory surface, but also to induce enhanced expression of cell surface molecules such as gC1qR. Enhanced expression of gC1qR in turn leads to: (i) high-affinity C1q binding and cell production of proinflammatory factors, and (ii) high-affinity HK binding and facilitation of the assembly of contact activation proteins leading to generation of bradykinin and possibly coagulation through activation of FXI.

Published

2006

158. Does C-2 kinin exist?

Author

Kaplan AP and Ghebrehiwet B

Subjects

Complement C1 Inactivator Proteins, Complement C1 Inhibitor Protein, Edema etiology, Serpins deficiency, Complement C2 metabolism, Kinins

Published

2005

159. Tissue factor pathway inhibitor-2 (TFPI-2) recognizes the complement and kininogen binding protein gC1qR/p33 (gC1qR): implications for vascular inflammation.

Author

Peerschke EI, Petrovan RJ, Ghebrehiwet B, and Ruf W

Subjects

Carrier Proteins, Complement C1q pharmacology, Fibrinolysin antagonists & inhibitors, Glycoproteins pharmacology, Humans, Hyaluronan Receptors pharmacology, Kallikreins antagonists & inhibitors, Kininogen, High-Molecular-Weight pharmacology, Mitochondrial Proteins, Protein Binding drug effects, Endothelium, Vascular pathology, Glycoproteins metabolism, Hyaluronan Receptors metabolism, Inflammation etiology

Abstract

Evidence is accumulating to suggest that TFPI-2 is involved in regulating pericellular proteases implicated in a variety of physiologic and pathologic processes including cancer cell invasion, vascular inflammation, and atherosclerosis. Recent immunohistochemical studies of advanced atherosclerotic lesions, demonstrated a similar tissue distribution for TFPI-2, High Molecular Weight Kininogen (HK), and gC1qR/p33 (gC1qR), a ubiquitously expressed, multicompartmental cellular protein involved in modulating complement, coagulation, and kinin cascades. Further studies to evaluate TFPI-2 interactions with gC1qR demonstrated direct interactions between gC1qR and TFPI-2 using immunoprecipitation and solid phase binding studies. Specific and saturable binding between TFPI-2 and gC1qR (estimated Kd: approximately 70 nM) was observed by ELISA and surface plasmon resonance (Biacore) binding assays. Binding was inhibited by antibodies to gC1qR, and was strongly dependent on the Kunitz-2 domain of TFPI-2, as deletion of this domain reduced gC1qR-TFPI-2 interactions by approximately 75%. Deletion of gC1qR amino acids 74-95, involved in C1q binding, had no effect on gC1qR binding to TFPI-2, although antibodies to this region and purified C1q both inhibited binding, most likely via allosteric effects. In contrast, HK did not affect TFPI-2 binding to gC1qR. Binding of TFPI-2 to gC1qR produced statistically significant but modest reductions in TFPI-2 inhibition of plasmin, but had no effect on kallikrein inhibition in fluid phase chromogenic assays. Taken together, these data suggest that gC1qR may participate in tissue remodeling and inflammation by localizing TFPI-2 to the pericellular environment to modulate local protease activity and regulate HK activation.

Published

2004

160. Receptor for the globular heads of C1q (gC1q-R, p33, hyaluronan-binding protein) is preferentially expressed by adenocarcinoma cells.

Author

Rubinstein DB, Stortchevoi A, Boosalis M, Ashfaq R, Ghebrehiwet B, Peerschke EI, Calvo F, and Guillaume T

Subjects

Base Sequence, Blotting, Northern, Breast Neoplasms metabolism, Carrier Proteins, Cell Line, Tumor, Cell Membrane metabolism, DNA, Complementary metabolism, Epitopes, Gene Library, Humans, Immunohistochemistry, Mitochondrial Proteins, Models, Biological, Molecular Sequence Data, Neoplasm Metastasis, Peptide Library, Protein Binding, RNA, Messenger metabolism, Sequence Homology, Nucleic Acid, Adenocarcinoma metabolism, Complement C1q biosynthesis, Hyaluronan Receptors biosynthesis, Membrane Glycoproteins, Receptors, Complement biosynthesis

Abstract

Combinatorial Ig libraries with phage display allow in vitro generation of human Ig fragments without the need to maintain hybridomas in ongoing cell culture or to select circulating Ig from human serum. Identifying tumor-associated antigens on the surface of intact tumor cells, as opposed to purified proteins, presents a challenge due to the difficulty of preserving complex 3-D epitopic sites on the cell surface, the variable expression of antigens on different malignant cell types and the stereotactic interference of closely associated proteins on the intact membrane surface limiting accessibility to antigenic sites. A combinatorial Ig library of 10(10) clones was generated from the cDNA of PBMCs derived from patients with breast adenocarcinoma. Following subtractive panning, the library was enriched for Ig (Fab fragment) binding to intact adenocarcinoma cells and the resultant Fabs were screened against a cDNA expression library, itself generated from breast cancer cells. Using this approach, we isolated clones from the cDNA library expressing gC1q-R, a glycoprotein comprising the major structure of C1, the first component of the complement system. gC1q-R is a 33 kDa glycoprotein expressed not only on the cell surface but also intracellularly, with motifs that target it to mitochondria and complete homology with HABP and human HeLa cell protein p32, which is copurified with pre-mRNA SF2. Sequencing of the gene encoding tumor-associated gC1q-R did not reveal any consistent tumor-specific mutations. However, histochemical staining with anti-gC1q-R MAb demonstrated marked differential expression of gC1q-R in thyroid, colon, pancreatic, gastric, esophageal and lung adenocarcinomas compared to their nonmalignant histologic counterparts. In contrast, differential expression was not seen in endometrial, renal and prostate carcinomas. Despite high expression in breast carcinoma, gC1q-R was also expressed in nonmalignant breast tissue. Although the precise relation of gC1q-R to carcinogenesis remains unclear, our finding of tumor overexpression and the known multivalent binding of gC1q-R to not only C1q itself but also a variety of circulating plasma proteins as well as its involvement in cell-to-cell interactions suggest that gC1q-R may have a role in tumor metastases and potentially serve in molecule-specific targeting of malignant cells., (Copyright 2004 Wiley-Liss, Inc.)

Published

2004

161. Interaction of high molecular weight kininogen binding proteins on endothelial cells.

Author

Joseph K, Tholanikunnel BG, Ghebrehiwet B, and Kaplan AP

Subjects

Binding Sites, Biotinylation, Blotting, Western, Cell Membrane metabolism, Cells, Cultured, Chromatography, Gel, Dose-Response Relationship, Drug, Electrophoresis, Polyacrylamide Gel, Endothelium, Vascular cytology, Enzyme-Linked Immunosorbent Assay, Factor XII metabolism, Humans, Keratins chemistry, Keratins metabolism, Kininogen, High-Molecular-Weight metabolism, Kininogens blood, Ligands, Membrane Glycoproteins metabolism, Precipitin Tests, Protein Binding, Receptors, Cell Surface metabolism, Receptors, Complement metabolism, Receptors, Urokinase Plasminogen Activator, Recombinant Proteins chemistry, Endothelial Cells metabolism, Kininogen, High-Molecular-Weight chemistry

Abstract

Cell surface proteins reported to participate in the binding and activation of the plasma kinin-forming cascade includes gC1qR, cytokeratin 1 and u-PAR. Each of these proteins binds high molecular weight kininogen (HK) as well as Factor XII. The studies on the interaction of these proteins, using dot-blot analysis, revealed that cytokeratin 1 binds to both gC1qR and u-PAR while gC1qR and u-PAR do not bind to each other. The binding properties of these proteins were further analyzed by gel filtration. When biotinylated cytokeratin 1 was incubated with either gC1qR or u-PAR and gel filtered, a new, higher molecular weight peak containing biotin was observed indicating complex formation. The protein shift was also similar to the biotin shift. Further, immunoprecipitation of solubilized endo-thelial cell plasma membrane proteins with anti-gC1qR recovered both gC1qR and cytokeratin 1, but not u-PAR. Immunoprecipitation with anti-u-PAR recovered only u-PAR and cytokeratin 1. By competitive ELISA, gC1qR inhibits u-PAR from binding to cytokeratin 1; u-PAR inhibits gC1qR binding to a lesser extent and requires a 10-fold molar excess. Our data suggest that formation of HK (and Factor XII) binding sites along endothelial cell membranes consists of bimolecular com-plexes of gC1qR-cytokeratin 1 and u-PAR-cytokeratin 1, with gC1qR binding being favored.

Published

2004

162. Complement component C1q induces endothelial cell adhesion and spreading through a docking/signaling partnership of C1q receptors and integrins.

Author

Ghebrehiwet B, Feng X, Kumar R, and Peerschke EI

Subjects

Antibodies, Monoclonal pharmacology, Biotin metabolism, Capillaries cytology, Capillaries drug effects, Cell Adhesion drug effects, Cell Division drug effects, Endothelium, Vascular drug effects, Enzyme-Linked Immunosorbent Assay, Epitopes drug effects, Epitopes metabolism, Humans, Integrin beta1 drug effects, Integrin beta1 metabolism, Kininogens metabolism, Microscopy, Fluorescence, Receptors, Cell Surface drug effects, Receptors, Cell Surface metabolism, Zinc pharmacology, Complement C1q pharmacology, Endothelium, Vascular cytology, Integrins metabolism, Receptors, Complement drug effects, Receptors, Complement metabolism

Abstract

The interaction of C1q with endothelial cells elicits a multiplicity of biologic responses. Although these specific responses are thought to be mediated by the interaction of C1q with proteins of the endothelial cell surface, the molecular identity of the participant(s) has not been clearly defined. In this study, we examined the role of two C1q-binding proteins, cC1q-R/CR and gC1q-R/p33, on C1q-mediated adhesion and spreading of human dermal microvascular endothelial cells (HDMVECs). A specific and dose-dependent adhesion and spreading was observed when HDMVECs were cultured in microtiter plate wells coated with concentrations of C1q ranging from 0 to 50 microg/ml. The extent of adhesion and spreading was similar to the adhesion seen on collagen-coated wells. Furthermore, the effect of C1q was mimicked by either polyclonal anti-cC1q-R or mAb 60.11, but not with isotype- and species-matched control IgG. More importantly, however, a 100% inhibition of spreading but not adhesion to C1q-coated wells was observed when HDMVECs were cultured in the presence of 30 mM of the peptide GRRGDSP but not GRRGESP. Furthermore, while anti-beta1 integrin antibody blocked adhesion and spreading, antialpha5 integrin only blocked spreading. Since earlier studies have shown that zinc induces the exposure of hydrophobic sites in the C-terminus of gC1q-R including the putative high-molecular weight kininogen (HK)-binding site corresponding to residues 204-218, we also examined the effect of zinc on antibody binding to cell surface gC1q-R. Flow cytometric data show that the binding of mAb 74.5.2, which recognizes residues 204-218, is greatly enhanced when endothelial cells were incubated in the presence of 50 microM zinc. In summary, our data show that: (a) C1q-mediated endothelial cell adhesion and spreading requires the cooperation of both C1q receptors and 1 integrins, and possibly other membrane-spanning molecules, and (b) zinc can induce the exposure of hydrophobic sites in the C-terminal domain of gC1q-R allowing a more efficient binding of mAb 74.5.2 and HK.

Published

2003

163. Maturation-dependent expression of C1q-binding proteins on the cell surface of human monocyte-derived dendritic cells.

Author

Vegh Z, Goyarts EC, Rozengarten K, Mazumder A, and Ghebrehiwet B

Subjects

Anti-Inflammatory Agents pharmacology, Apoptosis drug effects, Cells, Cultured, Culture Media, Cytokines metabolism, DNA, Complementary biosynthesis, DNA, Complementary genetics, Dexamethasone pharmacology, Down-Regulation drug effects, Flow Cytometry, Granulocyte-Macrophage Colony-Stimulating Factor metabolism, Humans, Indicators and Reagents, Lymphocyte Culture Test, Mixed, Microscopy, Confocal, Phenotype, Proteins genetics, RNA, Messenger biosynthesis, Reverse Transcriptase Polymerase Chain Reaction, Carrier Proteins, Dendritic Cells metabolism, Monocytes metabolism, Protein Biosynthesis, Receptors, Cell Surface metabolism

Abstract

The expression and cell surface levels of many important receptors are dependent on the maturation stage of dendritic cells (DCs), and related to the unique function of immature and mature DCs. In this report, we show for the first time that human monocyte-derived DCs express two types of C1q-receptors, gC1qR and cC1qR. Furthermore, immature DCs secrete detectable amount of C1q into the culture supernatant. Immature DCs express higher cell surface levels of both C1qRs than mature ones, while the total C1qR protein and mRNA levels remain the same. The following experimental evidence supports this conclusion. (1) Inflammatory cytokines and LPS, which induce maturation of DCs, downregulate surface expression of both C1qR molecules. (2) Cytokines and drugs (IL-10, IFNalpha, dexamethasone) that keep DCs phenotypically and functionally immature significantly upregulate the cell surface expression of both C1qRs. (3) Neither of these treatments changed the intracellular gC1qR level nor the gC1qR mRNA levels measured by real-time RT-PCR. The elevated surface expression of C1qRs on DCs has been found not to be due to increased apoptosis or cell death as the result of DC treatment. Taken together, these data show that human monocyte-derived DCs express gC1qR and cC1qR, their expression on the cell surface is maturation dependent and imature DCs secrete C1q. These data strongly suggest the role of C1qRs in immature DC function and in the regulation of immune processes.

Published

2003

164. Activation-dependent surface expression of gC1qR/p33 on human blood platelets.

Author

Peerschke EI, Murphy TK, and Ghebrehiwet B

Subjects

Adenosine Diphosphate pharmacology, Alprostadil pharmacology, Antibodies, Monoclonal immunology, Blood Platelets drug effects, Blood Platelets metabolism, Carrier Proteins, Chlorides pharmacology, Epinephrine pharmacology, Flow Cytometry, Humans, Mitochondrial Proteins, P-Selectin analysis, Peptide Fragments immunology, Platelet Activation drug effects, Protein Conformation drug effects, Proteins pharmacology, Receptors, Complement chemistry, Receptors, Complement immunology, Receptors, Thrombin, Serotonin metabolism, Zinc Compounds pharmacology, Hyaluronan Receptors, Membrane Glycoproteins, Platelet Activation physiology, Receptors, Complement physiology

Abstract

GC1qR/p33 (gC1qR) is expressed by a variety of somatic and cultured cells, including blood platelets. It interacts with several cellular, viral, bacterial, and plasma proteins, suggesting a potential role in thrombosis, inflammation, and infection. Considerable controversy has surrounded the surface membrane localization of gC1qR, however, since its cDNA sequence does not predict a traditional membrane-anchoring domain, and bears a typical mitochondrial targeting sequence. The present study examined gC1qR expression on resting and activated human blood platelets using flow cytometry and confocal microscopy with two monoclonal antibodies, 74.5.2 and 60.11, directed against gC1qR C-terminal amino acids 204-218, and N-terminal amino acids 76-93, respectively. Unstimulated platelets reacted minimally with either antibody. In contrast, platelet activation with TRAP, epinephrine, or ADP produced markedly increased gC1qR expression as reflected by 74.5.2 binding but not 60.11 binding. Platelet activation was verified using PAC-1 and anti CD 62 antibodies. Whereas PAC-1 binding to activated platelets could be reversed following platelet incubation with PGE1, 74.5.2 binding remained unchanged, suggesting the sustained expression of gC1qR following platelet stimulation. The data further demonstrate that detection of cell surface gC1qR may be dependent on antibody specificity. The ability of gC1qR to bind proteins involved in complement, coagulation, and kinin systems, as well as viral and bacterial pathogens including S. aureus protein A, supports the hypothesis that gC1qR expressed on activated platelets may contribute directly to thrombosis, inflammation, and endovascular infections.

Published

2003

165. The cytoplasmic tail peptide sequence of membrane type-1 matrix metalloproteinase (MT1-MMP) directly binds to gC1qR, a compartment-specific chaperone-like regulatory protein.

Author

Rozanov DV, Ghebrehiwet B, Ratnikov B, Monosov EZ, Deryugina EI, and Strongin AY

Subjects

Amino Acid Sequence, Binding Sites, Breast Neoplasms metabolism, Carrier Proteins, Cell Compartmentation, Cytoplasm metabolism, Humans, Matrix Metalloproteinases, Membrane-Associated, Mitochondrial Proteins, Molecular Sequence Data, Peptide Fragments metabolism, Precipitin Tests, Tumor Cells, Cultured, Hyaluronan Receptors, Membrane Glycoproteins, Metalloendopeptidases metabolism, Receptors, Complement metabolism

Abstract

Membrane type-1 matrix metalloproteinase (MT1-MMP), a key enzyme in cell locomotion, is known to be primarily recruited to the leading edge of migrating cells. This raises a possibility that the C-terminal cytoplasmic tail of MT1-MMP interacts with intracellular regulatory proteins, which modulate translocations of the protease across the cell. Here, we demonstrated that MT1-MMP via its cytoplasmic tail directly associates with a chaperone-like compartment-specific regulator gC1qR. Although a direct functional link between these two proteins remains uncertain, our observations suggest that the transient associations of gC1qR with the cytoplasmic tail of MT1-MMP are likely to be involved in the mechanisms regulating presentation of the protease at the tumor cell surface.

Published

2002

166. Zinc induces exposure of hydrophobic sites in the C-terminal domain of gC1q-R/p33.

Author

Kumar R, Peerschke EI, and Ghebrehiwet B

Subjects

Binding Sites, Carrier Proteins, Endothelium, Vascular cytology, Endothelium, Vascular metabolism, Humans, Hydrophobic and Hydrophilic Interactions, Kininogen, High-Molecular-Weight metabolism, Mitochondrial Proteins, Protein Conformation, Receptors, Complement metabolism, Hyaluronan Receptors, Membrane Glycoproteins, Receptors, Complement chemistry, Zinc pharmacology

Abstract

Endothelial cells and platelets are known to express gC1q-R on their surface. In addition to C1q, endothelial cell gC1q-R has been shown to bind high molecular weight kininogen (HK) and factor XII (FXII). However, unlike C1q, whose interaction with gC1q-R does not require divalent ions, the binding of HK to gC1q-R is absolutely dependent on the presence of zinc. However, the mechanism by which zinc modulates this interaction is not fully understood. To investigate the role of zinc, binding studies were done using the hydrophobic dye, bis-ANS. The fluorescence intensity of bis-ANS, greatly increases and the emission maximum is blue-shifted from 525 to 485nm upon binding to hydrophobic sites on proteins. In this report, we show that a blue-shift in emission maximum is also observed when bis-ANS binds to gC1q-R in the presence but not in the absence of zinc suggesting that zinc induces exposure of hydrophobic sites in the molecule. The binding of bis-ANS to gC1q-R is specific, dose-dependent, and reversible. In the presence of zinc, this binding is abrogated by monoclonal antibody 74.5.2 directed against gC1q-R residues 204-218. This segment of gC1q-R, which corresponds to the beta6 strand in the crystal structure, has been shown previously to be the binding site for HK. A similar trend in zinc-induced gC1q-R binding was also observed using the hydrophobic matrix octyl-Sepharose. Taken together, our data suggest that zinc can induce the exposure of hydrophobic sites in the C-terminal domain of gC1q-R involved in binding to HK/FXII.

Published

2002

167. The N-terminal conserved domain of rubella virus capsid interacts with the C-terminal region of cellular p32 and overexpression of p32 enhances the viral infectivity.

Author

Mohan KV, Ghebrehiwet B, and Atreya CD

Subjects

Amino Acid Sequence, Animals, Capsid genetics, Carrier Proteins, Chlorocebus aethiops, Conserved Sequence, Gene Expression, Membrane Glycoproteins genetics, Mitochondrial Proteins, Molecular Sequence Data, Protein Structure, Tertiary, Receptors, Complement genetics, Rubella virus genetics, Rubella virus metabolism, Vero Cells, Viral Vaccines genetics, Viral Vaccines metabolism, Capsid metabolism, Hyaluronan Receptors, Membrane Glycoproteins metabolism, Receptors, Complement metabolism, Rubella virus physiology

Abstract

Cellular 'defense collagens' are produced to launch virus-specific responses to clear the invading viruses. Cellular p32, the C1q binding protein is one such protein. In this report, we identified the interaction of p32 derived from a human lung diploid cell line (WI-38) with rubella virus capsid (RVCP from Therien strain) N-terminal 28-amino acid domain, which is conserved among several RV strains including the vaccine strains. We further identified that the C-terminal 69 aa of the mature p32 is sufficient to interact with the CP. In addition, we observed that in three independent Vero 76-derived cell lines constitutively overexpressing p32, the RV infectivity was enhanced. Our results suggest that RV has evolved a strategy whereby one of its proteins is recruited to interact with, and exploit the cellular defense machinery to its advantage.

Published

2002

168. The hemopexin-like C-terminal domain of membrane type 1 matrix metalloproteinase regulates proteolysis of a multifunctional protein, gC1qR.

Author

Rozanov DV, Ghebrehiwet B, Postnova TI, Eichinger A, Deryugina EI, and Strongin AY

Subjects

Amino Acid Sequence, Carrier Proteins, Catalytic Domain, Cells, Cultured, Computer Simulation, Female, Humans, Matrix Metalloproteinases, Membrane-Associated, Metalloendopeptidases metabolism, Mitochondrial Proteins, Molecular Sequence Data, Receptors, Complement chemistry, Tumor Cells, Cultured, Hyaluronan Receptors, Membrane Glycoproteins, Metalloendopeptidases chemistry, Receptors, Complement metabolism

Abstract

Matrix metalloproteinases (MMPs) including membrane type 1 MMP (MT1-MMP) can degrade extracellular matrix and cell surface receptor molecules and have an essential function in malignancy. Recently, we established a functional link between MT1-MMP and the receptor of complement component 1q (gC1qR). The gC1qR is known as a compartment-specific regulator of diverse cellular and viral proteins. Once released by proliferating cells, soluble gC1qR may inhibit complement component 1q hemolytic activity and play important roles in vivo in assisting tumor cells to evade destruction by complement. Here, we report that gC1qR is susceptible to MT1-MMP proteolysis in vitro and in cell cultures. The major MT1-MMP cleavage site (Gly(79) down arrow Gln(80)) is localized within the structurally disordered loop connecting the beta(3) and the beta(4) strands of gC1qR. The recombinant MT1-MMP construct that included the catalytic domain but lacked the hemopexin-like domain lost the proteolytic capacity; however, it retained the ability to bind gC1qR. Inhibition of MT1-MMP activity by a hydroxamate inhibitor converted the protease into a cell surface receptor of gC1qR and promoted co-precipitation MT1-MMP with the soluble gC1qR protein. It is tempting to hypothesize that these novel mechanisms may play important roles in vivo and have to be taken into account in designing hydroxamate-based cancer therapy.

Published

2002

169. Cooperation of C1q receptors and integrins in C1q-mediated endothelial cell adhesion and spreading.

Author

Feng X, Tonnesen MG, Peerschke EI, and Ghebrehiwet B

Subjects

Antibodies pharmacology, Calcium-Binding Proteins antagonists & inhibitors, Calcium-Binding Proteins immunology, Calreticulin, Carrier Proteins, Cells, Cultured, Complement C1q antagonists & inhibitors, Dermis blood supply, Dermis cytology, Endothelium, Vascular cytology, Endothelium, Vascular drug effects, Humans, Integrin beta1 immunology, Integrins physiology, Mitochondrial Proteins, Models, Immunological, Oligopeptides pharmacology, Receptors, Complement antagonists & inhibitors, Receptors, Complement immunology, Ribonucleoproteins antagonists & inhibitors, Ribonucleoproteins immunology, Calcium-Binding Proteins physiology, Cell Adhesion, Complement C1q pharmacology, Endothelium, Vascular immunology, Hyaluronan Receptors, Integrin beta1 physiology, Membrane Glycoproteins, Receptors, Complement physiology, Ribonucleoproteins physiology

Abstract

The interaction of C1q with endothelial cells elicits a multiplicity of biologic responses. Although these responses are presumed to be mediated by the interaction of C1q with endothelial cell surface proteins, the identity of the participants is not known. In this study we examined the roles of two C1q binding proteins, cC1q-R/calreticulin and gC1q-R/p33, in C1q-mediated adhesion and spreading of human dermal microvascular endothelial cells (HDMVEC). When HDMVEC were cultured in microtiter plate wells coated with concentrations of C1q ranging from 0 to 50 microg/ml, a specific and dose-dependent adhesion and spreading was observed. The extent of adhesion and spreading was similar to the adhesion seen on collagen-coated wells. Spreading (68 +/- 12%) and to a moderate extent adhesion (47 +/- 9%) were inhibited by anti-gC1q-R mAb 60.11. Similar effects were noted with polyclonal anti-cC1q-R but not with control nonimmune IgG. The two Abs had a slight additive effect (75 +/- 13% inhibition) when mixed together in the proportion of 100 microg/ml anti-gC1q-R and 30 microg/ml anti-cC1q-R. More importantly, a 100% inhibition of spreading, but not adhesion, to C1q-coated wells was observed when HDMVEC were cultured in the presence of 30 microM of the peptide GRRGDSP but not GRRGESP. Furthermore, while anti-beta(1) integrin Ab blocked both adhesion and spreading, anti-alpha(5) integrin blocked only spreading and not adhesion. Ag capture ELISA of endothelial cell membrane proteins using polyclonal anti-gC1q-R showed the presence of not only beta(1) and alpha(5) integrins but also CD44. Taken together these results suggest that endothelial cell adhesion and spreading require the cooperation of both C1qRs and beta(1) integrins and possibly other membrane-spanning molecules.

Published

2002

170. Surface expression of complement receptor gC1q-R/p33 is increased on the plasma membrane of human spermatozoa after capacitation.

Author

Grace KS, Bronson RA, and Ghebrehiwet B

Subjects

Antibodies, Monoclonal metabolism, Biotinylation, Blotting, Western, Carrier Proteins, Flow Cytometry, Fluorescein-5-isothiocyanate, Fluorescent Antibody Technique, Indirect, Fluorescent Dyes, Humans, Immunosorbent Techniques, Male, Microscopy, Confocal, Mitochondrial Proteins, Spermatozoa immunology, Spermatozoa physiology, Cell Membrane chemistry, Hyaluronan Receptors, Membrane Glycoproteins, Receptors, Complement analysis, Sperm Capacitation, Spermatozoa ultrastructure

Abstract

Evidence is increasing that complement components might play a role in fertilization. C1q, the first component of the classical complement cascade, has the ability to promote sperm agglutination in a capacitation-dependent manner as well as an effect on sperm-oolemma binding and fusion. We have previously detected gC1qR, the receptor for the globular head portion of C1q, on the surface of capacitated sperm. In this study, we examined the expression of gC1qR in both fresh and capacitated human spermatozoa. We performed immunoprecipitation for gC1qR and analyzed biotinylated sperm membrane by Western blot to illustrate an increase in receptor density after overnight capacitation. These results were confirmed by flow cytometric analysis of spermatozoa using fluorescein isothiocyanate-labeled monoclonal anti-gC1qR antibody. Confocal, indirect immunofluorescence microscopy revealed an increase in receptor expression over the rostral portion of the sperm head after capacitation. In addition, the ability of live spermatozoa to bind to monoclonal anti-gC1qR antibody-coated microtiter wells was also increased after capacitation. These results suggest that gC1qR may play a role in human fertilization.

Published

2002

171. C1q and mannose binding lectin engagement of cell surface calreticulin and CD91 initiates macropinocytosis and uptake of apoptotic cells.

Author

Ogden CA, deCathelineau A, Hoffmann PR, Bratton D, Ghebrehiwet B, Fadok VA, and Henson PM

Subjects

Calreticulin, Cells, Cultured, Collagen immunology, Collectins, Humans, Jurkat Cells, Low Density Lipoprotein Receptor-Related Protein-1, Monocytes cytology, Phagocytosis immunology, Signal Transduction immunology, Apoptosis immunology, Calcium-Binding Proteins immunology, Carrier Proteins immunology, Complement C1q immunology, Lectins immunology, Macrophages immunology, Pinocytosis immunology, Receptors, Immunologic immunology, Ribonucleoproteins immunology

Abstract

Removal of apoptotic cells is essential for maintenance of tissue homeostasis, organogenesis, remodeling, development, and maintenance of the immune system, protection against neoplasia, and resolution of inflammation. The mechanisms of this removal involve recognition of the apoptotic cell surface and initiation of phagocytic uptake into a variety of cell types. Here we provide evidence that C1q and mannose binding lectin (MBL), a member of the collectin family of proteins, bind to apoptotic cells and stimulate ingestion of these by ligation on the phagocyte surface of the multifunctional protein, calreticulin (also known as the cC1qR), which in turn is bound to the endocytic receptor protein CD91, also known as the alpha-2-macroglobulin receptor. Use of these proteins provides another example of apoptotic cell clearance mediated by pattern recognition molecules of the innate immune system. Ingestion of the apoptotic cells through calreticulin/CD91 stimulation is further shown to involve the process of macropinocytosis, implicated as a primitive and relatively nonselective uptake mechanism for C1q- and MBL-enhanced engulfment of whole, intact apoptotic cells, as well as cell debris and foreign organisms to which these molecules may bind.

Published

2001

172. The human gC1qR/p32 gene, C1qBP. Genomic organization and promoter analysis.

Author

Tye AJ, Ghebrehiwet B, Guo N, Sastry KN, Chow BK, Peerschke EI, and Lim BL

Subjects

3' Untranslated Regions genetics, 5' Untranslated Regions genetics, Base Sequence, Carrier Proteins, Cell Line, Complement C1q metabolism, Consensus Sequence, Exons, Genomic Library, Humans, Introns, Mitochondrial Proteins, Molecular Sequence Data, Protein Biosynthesis, Receptors, Complement chemistry, Receptors, Complement metabolism, Recombinant Proteins metabolism, Restriction Mapping, Sequence Deletion, TATA Box, Transfection, Hyaluronan Receptors, Membrane Glycoproteins, Promoter Regions, Genetic, Receptors, Complement genetics

Abstract

gC1qR is an ubiquitously expressed cell protein that interacts with the globular heads of C1q (gC1q) and many other ligands. In this study, the 7.8-kilobase pair (kb) human gC1qR/p32 (C1qBP) gene was cloned and found to consist of 6 exons and 5 introns. Analysis of a 1.3-kb DNA fragment at the 5'-flanking region of this gene revealed the presence of multiple TATA, CCAAT, and Sp1 binding sites. Luciferase reporter assays performed in different human cell lines demonstrated that the reporter gene was ubiquitously driven by this 1.3-kb fragment. Subsequent 5' and 3' deletion of this fragment confined promoter elements to within 400 base pairs (bp) upstream of the translational start site. Because the removal of the 8-bp consensus TATATATA at -399 to -406 and CCAAT at -410 to -414 did not significantly affect the transcription efficiency of the promoter, GC-rich sequences between this TATA box and the translation start site may be very important for the promoter activity of the C1qBP gene. One of seven GC-rich sequences in this region binds specifically to PANC-1 nuclear extracts, and the transcription factor Sp1 was shown to bind to this GC-rich sequence by the supershift assay. Primer extension analysis mapped three major transcription start regions. The farthest transcription start site is 49 bp upstream of the ATG translation initiation codon and is in close proximity of the specific SP1 binding site.

Published

2001

173. gC1q-R/p33, a member of a new class of multifunctional and multicompartmental cellular proteins, is involved in inflammation and infection.

Author

Ghebrehiwet B, Lim BL, Kumar R, Feng X, and Peerschke EI

Subjects

Amino Acid Motifs, Animals, Bacterial Proteins, Blood Platelets metabolism, Blood Proteins metabolism, Carrier Proteins, Cell Compartmentation, Cell Membrane metabolism, Chemotaxis, Chromosomes, Human, Pair 17 genetics, Complement C1q metabolism, Flow Cytometry, Gene Expression Regulation, Genes, Humans, Kininogen, High-Molecular-Weight metabolism, Ligands, Lymphocyte Activation, Membrane Proteins metabolism, Mice, Microscopy, Confocal, Mitochondria metabolism, Mitochondrial Proteins, Neoplasm Proteins physiology, Phagocytosis, Rats, Receptors, Complement chemistry, Receptors, Complement genetics, Receptors, Complement immunology, Signal Transduction, Staphylococcal Protein A metabolism, Structure-Activity Relationship, Subcellular Fractions metabolism, Tumor Cells, Cultured, Viral Proteins metabolism, Vitronectin metabolism, Hyaluronan Receptors, Infections metabolism, Inflammation metabolism, Membrane Glycoproteins, Receptors, Complement physiology

Abstract

Human gC1q-R (p33, p32, C1qBP, TAP) is a ubiquitously expressed, multiligand-binding, multicompartmental cellular protein involved in various ligand-mediated cellular responses. Although expressed on the surface of cells, an intriguing feature of the membrane-associated form of gC1q-R is that its translated amino acid sequence does not predict the presence of either a sequence motif compatible with a transmembrane segment or a consensus site for a glycosylphosphatidylinositol anchor. Moreover, the N-terminal sequence of the pre-pro-protein gC1q-R contains a motif that targets the molecule to the mitochondria and as such was deemed unlikely to be expressed on the surface. However, several lines of experimental evidence clearly show that gC1q-R is present in all compartments of the cell, including the extracellular cell surface. First, surface labeling of B lymphocytes with the membrane-impermeable reagent sulfosuccinimidyl 6-(biotinamido)hexanoate shows specific biotin incorporation into the surface-expressed but not the intracellular form of gC1q-R. Second, FACS and confocal laser scanning microscopic analyses using anti-gC1q-R IgG mAb 60.11 or 74.5.2, and the fluorophore Alexa 488-conjugated F(ab')2 goat anti-mouse IgG as a probe, demonstrated specific staining of Raji cells (>95% viable). Three-dimensional analyses of the same cells by confocal microscopy showed staining distribution that was consistent with surface expression. Third, endothelial gC1q-R, which is associated with the urokinase plasminogen activator receptor, and cytokeratin 1 bind 125I-high molecular weight kininogen in a specific manner, and the binding is inhibited dose-dependently by mAb 74.5.2 recognizing gC1q-R residues 204-218. Fourth, native gC1q-R purified from Raji cell membranes but not intracellular gC1q-R is glycosylated, as evidenced by a positive periodic acid Schiff stain as well as sensitivity to digestion with endoglycosidase H and F. Finally, cross-linking experiments using C1q as a ligand indicate that both cC1q-R and gC1q-R are co-immunoprecipitated with anti-C1q. Taken together, the evidence accumulated to date supports the concept that in addition to its intracellular localization, gC1q-R is expressed on the cell surface and can serve as a binding site for plasma and microbial proteins, but also challenges the existing paradigm that mitochondrial proteins never leave their designated compartment. It is therefore proposed that gC1q-R belongs to a growing list of a class of proteins initially targeted to the mitochondria but then exported to different compartments of the cell through specific mechanisms which have yet to be identified. The designation 'multifunctional and multicompartmental cellular proteins' is proposed for this class of proteins.

Published

2001

174. Human blood platelet gC1qR/p33.

Author

Peerschke EI and Ghebrehiwet B

Subjects

Bacterial Adhesion, Biotinylation, Blood Coagulation Factors metabolism, Carrier Proteins, Complement C1q metabolism, Humans, Kinins metabolism, Ligands, Mitochondrial Proteins, Platelet Aggregation, Protein Binding, Receptors, Complement blood, Receptors, Complement chemistry, Recombinant Fusion Proteins metabolism, Staphylococcal Infections immunology, Staphylococcal Protein A metabolism, Staphylococcus aureus immunology, Staphylococcus aureus pathogenicity, Staphylococcus aureus physiology, Virulence, Blood Platelets immunology, Hyaluronan Receptors, Membrane Glycoproteins, Receptors, Complement physiology

Abstract

Platelets are involved in the development of many types of vascular lesions. In addition to their role in primary hemostasis, they participate in inflammatory processes that may contribute to the development of thrombosis, atherosclerosis and vasculitis. In this regard, we have been interested in platelet interactions with the complement subcomponent C1q. C1q has been shown to modulate platelet interactions with collagen and immune complexes, and has been identified at sites of vascular injury and inflammation, as well as in atherosclerotic lesions. Platelets express a variety of C1q binding sites, including gC1qR/p33 (gC1qR), a multifunctional, multicompartment cellular protein. Here we focus on the structure and function of platelet gC1qR and its emerging role in modulating platelet function at sites of vascular injury and inflammation.

Published

2001

175. Factor XII-dependent contact activation on endothelial cells and binding proteins gC1qR and cytokeratin 1.

Author

Joseph K, Shibayama Y, Ghebrehiwet B, and Kaplan AP

Subjects

Carrier Proteins, Complement C1 Inactivator Proteins pharmacology, Dose-Response Relationship, Drug, Endothelium, Vascular chemistry, Endothelium, Vascular cytology, Factor XII drug effects, Humans, Keratins metabolism, Kinetics, Kininogen, High-Molecular-Weight pharmacology, Membrane Proteins metabolism, Mitochondrial Proteins, Molecular Chaperones metabolism, Molecular Chaperones pharmacology, Prekallikrein metabolism, Prekallikrein pharmacology, Umbilical Veins cytology, Zinc pharmacology, Endothelium, Vascular metabolism, Factor XII metabolism, Factor XII pharmacology, Hyaluronan Receptors, Kallikrein-Kinin System drug effects, Keratins pharmacology, Membrane Glycoproteins, Receptors, Complement metabolism

Abstract

Although proteins of the kinin-forming pathway are bound along the surface of endothelial cells, the mechanism of activation of this proteolytic cascade is unclear. Endothelial cell surface proteins, gC1qR and cytokeratin 1, are capable of binding Factor XII and high molecular weight kininogen (HK) in a zinc-dependent reaction thus we considered the possibility that these proteins might catalyze initiation of the cascade. Incubation of Factor XII, prekallikrein, and HK with gC1qR or cytokeratin 1 leads to a zinc-dependent and Factor XII-dependent conversion of prekallikrein to kallikrein. We also demonstrate that normal plasma is capable of activating upon interaction with the cells whereas plasma deficient in Factor XII, prekallikrein and HK do not activate. Normal plasma activation was inhibitable by antibody to gC1qR and cytokeratin 1. Thus, gC1qR and cytokeratin 1, represent potential initiating surfaces for activation of the plasma kinin-forming cascade and may do so as a result of their expression along cell surfaces.

Published

2001

176. Activation of the kinin-forming cascade on the surface of endothelial cells.

Author

Joseph K, Ghebrehiwet B, and Kaplan AP

Subjects

Antibodies, Blocking pharmacology, Cell Line, Endothelium, Vascular cytology, Endothelium, Vascular drug effects, Factor XII pharmacology, Humans, Kininogens pharmacology, Kinins physiology, Molecular Weight, Prekallikrein pharmacology, Receptors, Cell Surface metabolism, Endothelium, Vascular metabolism, Kinins biosynthesis

Abstract

Activation of the plasma kallikrein-kinin forming cascade takes place upon incubation with human umbilical vein endothelial cells. The mechanism by which initiation occurs is uncertain. Zinc-dependent binding of plasma proteins to gC1qR, cytokeratin 1, and perhaps u-PAR is requisite for activation to take place. We demonstrate here that during a 2 hour incubation time plasma deficient in either factor XII or high molecular weight kininogen (HK) fails to activate, as compared to normal plasma, but with more prolonged incubation, factor XII-deficient plasma gradually activates while HK-deficient plasma does not. Our data support both factor XII-dependent (rapid) and factor XII-independent (slow) mechanisms; the latter may require a cell-derived protease to activate prekallikrein and the presence of zinc ions and HK.

Published

2001

177. Activation of the plasma kinin forming cascade along cell surfaces.

Author

Kaplan AP, Joseph K, Shibayama Y, Reddigari S, and Ghebrehiwet B

Subjects

Carrier Proteins, Cells, Cultured, Factor XII metabolism, Humans, Keratins metabolism, Membrane Proteins metabolism, Mitochondrial Proteins, Prekallikrein metabolism, Receptors, Complement metabolism, Endothelium, Vascular metabolism, Hyaluronan Receptors, Kininogen, High-Molecular-Weight metabolism, Membrane Glycoproteins

Abstract

Proteins of the plasma kinin-forming cascade bind to endothelial cells and activation of the cascade can be initiated along the surface. The light chain of high molecular weight kininogen (HK) (domain 5) and factor XII bind to gC1qR, the heavy chain of HK (domain 3) binds to cytokeratin 1 and the interactions are zinc dependent. Prekallikrein binds to domain 6 of HK. Antisera to gC1qR and cytokeratin 1 inhibit binding and activation. Incubation of normal plasma with endothelial cells leads to gradual conversion of prekallikrein to kallikrein, while plasma deficient in factor XII or HK are inactive within a 2-hour time frame. Thus factor XII is critical for activation to proceed. Augmentation of these reactions may occur when C1 inhibitor is functionally deficient or with ACE inhibitors which also inhibit kininases., (Copyright 2001 S. Karger AG, Basel)

Published

2001

178. Protein kinase C [micro] is regulated by the multifunctional chaperon protein p32.

Author

Storz P, Hausser A, Link G, Dedio J, Ghebrehiwet B, Pfizenmaier K, and Johannes FJ

Subjects

Animals, B-Lymphocytes, Binding Sites, Carrier Proteins, Cell Line, Cloning, Molecular, Glutathione Transferase, Golgi Apparatus metabolism, Humans, JNK Mitogen-Activated Protein Kinases, Mitochondria metabolism, Mitochondrial Proteins, Mitogen-Activated Protein Kinases metabolism, Protein Binding, Recombinant Fusion Proteins metabolism, Saccharomyces cerevisiae genetics, Saccharomyces cerevisiae growth & development, Spodoptera, Transfection, Hyaluronan Receptors, Membrane Glycoproteins, Molecular Chaperones metabolism, Protein Kinase C metabolism, Receptors, Complement metabolism

Abstract

We identified the multifunctional chaperon protein p32 as a protein kinase C (PKC)-binding protein interacting with PKCalpha, PKCzeta, PKCdelta, and PKC mu. We have analyzed the interaction of PKC mu with p32 in detail, and we show here in vivo association of PKC mu, as revealed from yeast two-hybrid analysis, precipitation assays using glutathione S-transferase fusion proteins, and reciprocal coimmunoprecipitation. In SKW 6.4 cells, PKC mu is constitutively associated with p32 at mitochondrial membranes, evident from colocalization with cytochrome c. p32 interacts with PKC mu in a compartment-specific manner, as it can be coimmunoprecipitated mainly from the particulate and not from the soluble fraction, despite the presence of p32 in both fractions. Although p32 binds to the kinase domain of PKC mu, it does not serve as a substrate. Interestingly, PKC mu-p32 immunocomplexes precipitated from the particulate fraction of two distinct cell lines, SKW 6.4 and 293T, show no detectable substrate phosphorylation. In support of a kinase regulatory function of p32, addition of p32 to in vitro kinase assays blocked, in a dose-dependent manner, aldolase but not autophosphorylation of PKC mu, suggesting a steric hindrance of substrate within the kinase domain. Together, these findings identify p32 as a novel, compartment-specific regulator of PKC mu kinase activity.

Published

2000

179. gC1q-R/p32, a C1q-binding protein, is a receptor for the InlB invasion protein of Listeria monocytogenes.

Author

Braun L, Ghebrehiwet B, and Cossart P

Subjects

Adaptor Proteins, Signal Transducing, Amino Acid Sequence, Animals, Antibodies pharmacology, Bacterial Proteins genetics, Base Sequence, Binding, Competitive, Carrier Proteins, Cell Line, Chlorocebus aethiops, DNA Primers genetics, HeLa Cells, Humans, Listeria monocytogenes genetics, Listeria monocytogenes pathogenicity, Membrane Proteins genetics, Mitochondrial Proteins, Molecular Sequence Data, Phosphoproteins metabolism, Phosphorylation, Receptors, Complement antagonists & inhibitors, Receptors, Complement genetics, Transfection, Tyrosine metabolism, Vero Cells, Bacterial Proteins metabolism, Complement C1q metabolism, Hyaluronan Receptors, Listeria monocytogenes metabolism, Membrane Glycoproteins, Membrane Proteins metabolism, Receptors, Complement metabolism

Abstract

InlB is a Listeria monocytogenes protein that promotes entry of the bacterium into mammalian cells by stimulating tyrosine phosphorylation of the adaptor proteins Gab1, Cbl and Shc, and activation of phosphatidyl- inositol (PI) 3-kinase. Using affinity chromatography and enzyme-linked immunosorbent assay, we demonstrate a direct interaction between InlB and the mammalian protein gC1q-R, the receptor of the globular part of the complement component C1q. Soluble C1q or anti-gC1q-R antibodies impair InlB-mediated entry. Transient transfection of GPC16 cells, which are non-permissive to InlB-mediated entry, with a plasmid-expressing human gC1q-R promotes entry of InlB-coated beads. Furthermore, several experiments indicate that membrane recruitment and activation of PI 3-kinase involve an InlB-gC1q-R interaction and that gC1q-R associates with Gab1 upon stimulation of Vero cells with InlB. Thus, gC1q-R constitutes a cellular receptor involved in InlB-mediated activation of PI 3-kinase and tyrosine phosphorylation of the adaptor protein Gab1. After E-cadherin, the receptor for internalin, gC1q-R is the second identified mammalian receptor promoting entry of L. monocytogenes into mammalian cells.

Published

2000

180. Cytokeratin 1 and gC1qR mediate high molecular weight kininogen binding to endothelial cells.

Author

Joseph K, Ghebrehiwet B, and Kaplan AP

Subjects

Amino Acid Sequence, Biotinylation, Carrier Proteins, Complement C1q metabolism, Humans, Iodine Radioisotopes, Keratins chemistry, Ligands, Mitochondrial Proteins, Peptide Fragments chemistry, Protein Binding drug effects, Umbilical Veins cytology, Zinc metabolism, Endothelium, Vascular cytology, Hyaluronan Receptors, Keratins pharmacology, Kininogen, High-Molecular-Weight metabolism, Membrane Glycoproteins, Receptors, Complement physiology

Abstract

High molecular weight kininogen (HK) attaches to endothelial cells by separate sites on the heavy and light chains and requires 15-50 microM zinc. Previously identified binding proteins include gC1qR, cytokeratin 1, and the urokinase plasminogen activator receptor; however, their relative contributions to binding are not yet clarified. We have prepared affinity columns to which were coupled either cleaved HK or peptide LDCNAEVYVVPWEKKIYPTVNCQPLGM derived from heavy-chain domain 3. Endothelial cell membranes were solubilized and chromatographed in the presence or absence of zinc ion, the bound proteins were eluted, and active fractions were identified by dot blot using biotinylated HK, SDS/PAGE, and Western blot analysis. The peptide containing column eluate revealed but one band at 68 kDa if zinc ion was present which was identified as cytokeratin 1 by amino acid sequencing of an internal peptide. The HK affinity column revealed bands at 68 kDa (cytokeratin 1), 33 kDa (gC1qR), and 66 kDa (unidentified). HK or domain 3-derived peptide bound to the 68 kDa band; prekallikrein and Factor XII did not. HK or Factor XII bound to the 33-kDa band if zinc was present while no binding to the 66 kDa band was observed. Antibody to cytokeratin 1 inhibited HK binding to endothelial cells by 30%, antibody to gC1qR inhibited HK binding to endothelial cells by 72%, and a mixture of both inhibited binding by 86%. Our data suggest HK binding by interaction of the heavy-chain domain 3 with cytokeratin 1 and the light chain with gC1qR., (Copyright 1999 Academic Press.)

Published

1999

181. Interaction of factor XII and high molecular weight kininogen with cytokeratin 1 and gC1qR of vascular endothelial cells and with aggregated Abeta protein of Alzheimer's disease.

Author

Joseph K, Shibayama Y, Nakazawa Y, Peerschke EI, Ghebrehiwet B, and Kaplan AP

Subjects

Animals, Bradykinin biosynthesis, Carrier Proteins, Humans, Mitochondrial Proteins, Amyloid beta-Peptides metabolism, Endothelium, Vascular metabolism, Factor XII metabolism, Hyaluronan Receptors, Keratins metabolism, Kininogen, High-Molecular-Weight metabolism, Membrane Glycoproteins, Receptors, Complement metabolism

Abstract

High molecular weight kininogen (HK) attaches to endothelial cells at separate sites on the heavy and light chains by a process which requires 15-50 microM zinc. Previously identified binding proteins include gClqR, cytokeratin 1, and the urokinase plasminogen activator receptor (U-par), however, their relative contribution to binding are not yet clarified. We have purified the binding proteins by affinity chromatography, in the presence of zinc ion, and identified cytokeratin 1 and gC1qR by amino acid sequencing of an internal peptide and by immunoblot as heavy chain and light chain binding proteins, respectively. Antibody to cytokeratin 1 inhibited HK binding to endothelial cells by 30%, antibody to gClqR inhibited HK binding to endothelial cells by 72%, and a mixture of both inhibited binding by 86%. The binding and activation of the proteins of the kinin-forming cascade along the cell surface is zinc-dependent. Similarly, proteins of the plasma kinin-forming cascade can be activated by binding to aggregated A(beta) protein of Alzheimer's disease. Activation of the cascade using purified proteins or upon addition of Abeta to plasma requires aggregation of A(beta) and the reactions are zinc-dependent. In plasma, HK is cleaved and bradykinin is liberated. The data demonstrate that aggregated A(beta) can bind and activate proenzymes of the plasma kinin-forming cascade to release bradykinin and these reactions are dependent on zinc ion.

Published

1999

182. Platelet glycoprotein Ib: a zinc-dependent binding protein for the heavy chain of high-molecular-weight kininogen.

Author

Joseph K, Nakazawa Y, Bahou WF, Ghebrehiwet B, and Kaplan AP

Subjects

Antibodies, Biotinylation, Cell Membrane metabolism, Chromatography, Affinity, Electrophoresis, Polyacrylamide Gel, Humans, Kinetics, Molecular Weight, Platelet Glycoprotein GPIb-IX Complex immunology, Platelet Glycoprotein GPIb-IX Complex isolation & purification, Thrombin metabolism, Zinc pharmacology, Blood Platelets metabolism, Factor XII metabolism, Kininogen, High-Molecular-Weight blood, Platelet Glycoprotein GPIb-IX Complex metabolism, Zinc metabolism

Abstract

Domains 3 and 5 of high-molecular-weight kininogen (HK) have been shown to bind to platelets in a zinc-dependent reaction. However, the platelet-binding proteins responsible for this interaction have not been identified. We have focused on the platelet-binding site for the heavy chain (domain 3), which we approached using a domain 3-derived peptide ligand and isolated binding proteins by affinity chromatography. The domain 3-derived peptide, thrombin, HK, factor XII, as well as antibody to glycocalicin (the N-terminal portion of the alpha chain of GPIb) recognized a protein at 74 kD. We also isolated the thrombin receptor (PAR 1) at 45 kD, however, none of the above-mentioned ligands bound to this protein. Isolation of platelet membrane proteins using a monoclonal anti-glycocalicin antibody column revealed the same HK binding protein at 74 kD, which was reactive with anti-GPIb and represents a GPIb fragment. By photoaffinity labeling, HK interacted with membrane GPIb, which was then isolated in native form (135 kD) along with gC1qR, a ligand for the HK light chain. Finally, (125)I-HK binding to platelets was significantly inhibited by the anti-GPIb antibody. These results suggest that the GPIb alpha chain, a known thrombin binding protein, is also one of the zinc-dependent platelet membrane binding sites for HK domain 3.

Published

1999

183. Up-regulation of endothelial cell binding proteins/receptors for complement component C1q by inflammatory cytokines.

Author

Guo WX, Ghebrehiwet B, Weksler B, Schweitzer K, and Peerschke EI

Subjects

Blotting, Northern, Blotting, Western, Bone Marrow Cells metabolism, Bone Marrow Cells physiology, Carrier Proteins, Cell Division, Cell Line, Cytokines pharmacology, Endothelium, Vascular cytology, Escherichia coli chemistry, Humans, Interferon-gamma pharmacology, Lipopolysaccharides pharmacology, Microcirculation, Mitochondrial Proteins, RNA, Messenger metabolism, Recombinant Proteins, Tumor Necrosis Factor-alpha pharmacology, Up-Regulation, Complement C1q metabolism, Cytokines physiology, Endothelium, Vascular metabolism, Hyaluronan Receptors, Inflammation metabolism, Membrane Glycoproteins, Receptors, Complement metabolism

Abstract

Endothelial cells express a variety of receptor systems involved in humoral defense, including receptors for the collagen-like and globular domains of the complement component C1q, designated cC1qR and gC1qR, respectively. In the present study a microvascular endothelial cell line was used to test the hypothesis that expression of these C1q-binding proteins may be affected by vascular inflammatory reactions. The results demonstrate that the expression of both cC1qR and gC1qR by bone marrow vascular endothelial cells is up-regulated by inflammatory mediators, interferon-gamma, tumor necrosis factor-alpha, and lipopolysaccharide (Escherichia coli, 055:B5) in a dose- and time-dependent manner, as detected by enzyme-linked immunosorbent assay. cC1qR and gC1qR expression increased significantly (P < .05) within 4 to 7 hours and doubled after 22 hours of stimulation. 3H-thymidine incorporation studies and direct cell counts confirmed that increased C1qR expression was not due to increased cell proliferation. Northern blot analysis revealed that the up-regulation of cC1qR and gC1qR protein expression was preceded by increases in corresponding mRNA levels, suggesting increased gene transcription. Indeed C1qR mRNA up-regulation was prevented by actinomycin D, and C1qR protein synthesis was inhibited by cycloheximide. Bone marrow vascular endothelial cell exposure to C1q, however, did not alter cC1qR or gC1qR expression, but up-regulation of the leukocyte adhesion molecule ICAM-1 was noted in the presence of aggregated C1q. The up-regulation of C1qR by inflammatory mediators and the ability of C1q itself to increase ICAM-1 expression suggest a potential role for these binding sites in vascular inflammation and immune injury.

Published

1999

184. The receptor for the globular "heads" of C1q, gC1q-R, binds to fibrinogen/fibrin and impairs its polymerization.

Author

Lu PD, Galanakis DK, Ghebrehiwet B, and Peerschke EI

Subjects

Anticoagulants metabolism, Binding Sites, Blood Coagulation, Carrier Proteins, Cations, Divalent pharmacology, Complement Activation, Humans, Mitochondrial Proteins, Peptide Fragments metabolism, Protein Binding drug effects, Receptors, Complement genetics, Recombinant Proteins metabolism, Complement C1q metabolism, Fibrin metabolism, Fibrinogen metabolism, Hyaluronan Receptors, Inflammation Mediators metabolism, Membrane Glycoproteins, Receptors, Complement metabolism

Abstract

The 33-kDa cellular C1q binding protein, designated gC1q-R was previously shown to bind a number of plasma proteins involved in the coagulation and kinin systems. This study demonstrates the interaction between recombinant gC1q-R and fibrinogen. Using enzyme-linked immunosorbent assays, biotinylated gC1q-R was found to bind to microplate-immobilized fibrinogen in a manner which was specific and inhibited by excess soluble fibrinogen or polyclonal antibodies directed against either gC1q-R or fibrinogen. Moreover, gC1q-R inhibited fibrin polymerization in a dose-dependent manner. Reptilase induced fibrin clot formation was completely inhibited by gC1q-R at a 2:1 molar ratio (gC1q-R:fibrinogen), and repolymerization of thrombin induced fibrin monomers was similarly abrogated. At equivalent molar concentrations, gC1q-R appeared to be a more potent inhibitor of fibrin polymerization than fibrinogen, a well-known inhibitor. Moreover, in the presence of both gC1q-R and soluble fibrinogen, the effect of each inhibitor on fibrin polymerization was additive. When plasmin derived fibrinogen degradation products, including the C-terminal D domain (D-100) or the N-terminal E domain, were immobilized on microtiter plates, gC1q-R bound to fibrinogen fragment D-100, but not to fragment E. Further digestion of fibrinogen fragment D-100 by plasmin to fragment D-60 resulted in loss of gC1q-R binding. Thus, gC1q-R binds to the D domain of fibrinogen/fibrin, and the carboxyterminal segment of at least the fibrinogen/fibrin gamma chain appears important for this interaction. These observations may suggest a potential role for gC1q-R in modulating fibrin formation particularly at local sites of immune injury or inflammation., (Copyright 1999 Academic Press.)

Published

1999

185. Bradykinin formation. Plasma and tissue pathways and cellular interactions.

Author

Kaplan AP, Joseph K, Shibayama Y, Nakazawa Y, Ghebrehiwet B, Reddigari S, and Silverberg M

Subjects

Animals, Blood Platelets metabolism, Bradykinin blood, Bradykinin physiology, Endothelium, Vascular cytology, Endothelium, Vascular metabolism, Enzyme Precursors metabolism, Factor XI metabolism, Humans, Kallikreins biosynthesis, Kallikreins metabolism, Kininogens chemistry, Kininogens genetics, Kininogens metabolism, Neutrophils metabolism, Tissue Kallikreins, Bradykinin biosynthesis, Kallikrein-Kinin System physiology

Published

1998

186. Platelet receptors for the complement component C1q: implications for hemostasis and thrombosis.

Author

Peerschke EI and Ghebrehiwet B

Subjects

Animals, Antigen-Antibody Complex blood, Binding Sites, Carrier Proteins, Humans, Mitochondrial Proteins, Blood Platelets physiology, Complement C1q metabolism, Hemostasis physiology, Hyaluronan Receptors, Membrane Glycoproteins, Receptors, Complement physiology, Thrombosis physiopathology

Abstract

Platelets participate in a variety of responses of the blood to injury (1). In addition to their well known role in hemostasis and thrombosis, platelets play a role in inflammation and react with components of the immune system. Immune complexes and aggregated IgG, for example, are known to activate platelets via ligation of Fc gamma RII receptors and induce the release of platelet granule contents, including biogenic amines and adenine nucleotides (2). Platelets also interact with the complement subcomponent C1q utilizing binding sites that are unrelated to C1s, a complement subcomponent which was originally suggested to support C1q binding to thrombocytes (3). The physiologic and pathologic consequences of platelet C1q receptor occupancy are incompletely understood. Platelet C1q receptors may contribute to immune complex localization and clearance, as has been suggested for C1q receptors on phagocytic cells (4), but considerable evidence is emerging to suggest that the interaction between C1q and platelets may influence hemostasis and perhaps, more profoundly, thrombotic complications resulting from immune injury. This review will summarize current concepts in C1q receptor biology as it relates to human platelet function and blood coagulation.

Published

1998

187. Structure and function of gC1q-R: a multiligand binding cellular protein.

Author

Ghebrehiwet B and Peerschke EI

Subjects

Animals, Carrier Proteins, Chromosomes, Human, Pair 17 genetics, Cloning, Molecular, Factor XII metabolism, Humans, Kininogen, High-Molecular-Weight metabolism, Ligands, Mice, Mitochondrial Proteins, Receptors, Complement chemistry, Receptors, Complement genetics, Thrombin metabolism, Vitronectin metabolism, Complement C1q metabolism, Hyaluronan Receptors, Membrane Glycoproteins, Receptors, Complement physiology

Abstract

gC1q-R is a 33 kDa, single chain, highly acidic protein, which was first isolated from membrane preparation of Raji cells and now appears to be ubiquitously distributed. Although, gC1q-R was originally identified as a protein which binds to the globular "heads" of C1q, recent evidence suggests that the molecule is in fact a multiligand binding, multifunctional protein with affinity for diverse ligands which at best are functionally related. These molecules include: thrombin, vitronectin, and high molecular weight kininogen. The gC1q-R molecule, which is identical to the transcription factors SF2 and the Tat-associated protein, or TAP, is the product of a single gene localized on chromosome 17p13.3 in human, and chromosome 11 in mouse, and is encoded by an approximately 1.5-1.6 kb mRNA. The full length cDNA encodes a primary translation protein of 282 residues and the 'mature' or membrane form of the protein isolated from Raji cells corresponds to residues 74-282 and is presumed to be generated by a site-specific cleavage and removal of the highly basic, 73-residues long, N-terminal segment during post-translational processing. The translated amino acid sequence does not predict for the presence of a conventional sequence motif compatible with a transmembrane segment and does not have a consensus site for a GPI anchor. However, there is strong evidence which indicates that gC1q-R is expressed both inside the cell and on the membrane. First, certain mAbs raised against gC1q-R react moderately with intact Raji cells in suspension and this binding increases when the cells are first bound to poly-L-lysine coated surfaces and then fixed with glutaraldehyde. Second, surface labeling of cells using the membrane impermeable sulfo-NHS-LC-biotin shows that gC1q-R on the surface incorporates biotin whereas intracellular gC1q-R does not. In addition, the membrane expression of gC1q-R can be upregulated with inflammatory cytokines such as INF-gamma, TNF-alpha, or LPS. These results suggest, that gC1q-R, is localized both as an intracellular and as a cell surface protein and may have important biological functions in both compartments of the cell.

Published

1998

188. Complement C1q inhibits cellular spreading and stimulates adenylyl cyclase activity of fibroblasts.

Author

Tan X, Wong ST, Ghebrehiwet B, Storm DR, and Bordin S

Subjects

Carrier Proteins, Cells, Cultured, Complement C1q physiology, Cyclic AMP metabolism, Enzyme Activation, Fibroblasts cytology, Fibronectins metabolism, Gingiva cytology, Gingiva drug effects, Gingiva enzymology, Humans, Mitochondrial Proteins, Receptors, Complement metabolism, Adenylyl Cyclases metabolism, Complement C1q pharmacology, Fibroblasts drug effects, Fibroblasts enzymology, Hyaluronan Receptors, Membrane Glycoproteins

Abstract

C1q selectively localizes at injured tissues, where it may function as a regulator of cell-matrix interactions. We show here that purified C1q, added to the culture medium of human gingival fibroblasts (HF) spread onto fibronectin substrates, elicited a round morphology that was accompanied by altered F-actin and correlated with inhibition of cellular spreading. Shape modification required integrity of the molecule and was specific, dose dependent, nontoxic, and reversible. Antispreading activity was mediated, at least in part, by specific cell-surface C1q receptors. We hypothesized that ligand occupancy of C1q receptors could influence shape by affecting intracellular levels of cyclic AMP (cAMP). Within 20 min of exposure of adhering HF to C1q, we detected an increase in adenylyl cyclase activity (six- to ninefold) in cAMP accumulation (by 20%) and in cAMP-dependent protein kinase activity (by 20%). These changes suggested that the rounding effect of C1q may be associated with activation of the adenylyl cyclase pathway.

Published

1998

189. C1q-mediated chemotaxis by human neutrophils: involvement of gClqR and G-protein signalling mechanisms.

Author

Leigh LE, Ghebrehiwet B, Perera TP, Bird IN, Strong P, Kishore U, Reid KB, and Eggleton P

Subjects

Androstadienes pharmacology, Carrier Proteins, Chromones pharmacology, Collagen chemistry, Enzyme Inhibitors pharmacology, Humans, Mitochondrial Proteins, Morpholines pharmacology, Pertussis Toxin, Phosphoinositide-3 Kinase Inhibitors, Signal Transduction, Virulence Factors, Bordetella pharmacology, Wortmannin, Chemotaxis, Leukocyte drug effects, Complement C1q physiology, GTP-Binding Proteins physiology, Hyaluronan Receptors, Membrane Glycoproteins, Neutrophils physiology, Receptors, Complement physiology

Abstract

C1q, the first component of the classical pathway of the complement system, interacts with various cell types and triggers a variety of cell-specific cellular responses, such as oxidative burst, chemotaxis, phagocytosis, etc. Different biological responses are attributed to the interaction of C1q with more than one putative cell-surface C1q receptor/C1q-binding protein. Previously, it has been shown that C1q-mediated oxidative burst by neutrophils is not linked to G-protein-coupled fMet-Leu-Phe-mediated response. In the present study, we have investigated neutrophil migration brought about by C1q and tried to identify the signal-transduction pathways involved in the chemotactic response. We found that C1q stimulated neutrophil migration in a dose-dependent manner, primarily by enhancing chemotaxis (directed movement) rather than chemokinesis (random movement). This C1q-induced chemotaxis could be abolished by an inhibitor of G-proteins (pertussis toxin) and PtdIns(3,4,5)P3 kinase (wortmannin and LY294002). The collagen tail of C1q appeared to mediate chemotaxis. gC1qR, a C1q-binding protein, has recently been reported to participate in C1q-mediated chemotaxis of murine mast cells and human eosinophils. We observed that gC1qR enhanced binding of free C1q to adherent neutrophils and promoted C1q-mediated chemotaxis of neutrophils by nearly seven-fold. Our results suggests C1q-mediated chemotaxis involves gC1qR as well as G-protein-coupled signal-transduction mechanisms operating downstream to neutrophil chemotaxis.

Published

1998

190. Characterisation of the rat and mouse homologues of gC1qBP, a 33 kDa glycoprotein that binds to the globular 'heads' of C1q.

Author

Lynch NJ, Reid KB, van den Berg RH, Daha MR, Leigh LA, Ghebrehiwet B, Lim WB, and Schwaeble WJ

Subjects

Amino Acid Sequence, Animals, Binding Sites, Carrier Proteins, Cerebral Cortex metabolism, Gene Library, Humans, Liver metabolism, Macrophages metabolism, Membrane Glycoproteins biosynthesis, Mice, Mitochondrial Proteins, Molecular Sequence Data, Molecular Weight, Rats, Receptors, Complement biosynthesis, Recombinant Proteins biosynthesis, Recombinant Proteins chemistry, Sequence Alignment, Sequence Homology, Amino Acid, Complement C1q chemistry, Complement C1q metabolism, Hyaluronan Receptors, Membrane Glycoproteins chemistry, Receptors, Complement chemistry

Abstract

gC1qBP is a 33 kDa glycoprotein that binds to the globular 'heads' of C1q. We have cloned cDNAs encoding the rat and mouse homologues of gC1qBP. Comparison of the cDNA-derived amino acid sequences of gC1qBP reveals that either of the rodent sequences is 89.9% identical to the reported human sequence. Recombinant rat gC1qBP binds avidly to human C1q. gC1qBP mRNA is abundantly expressed in every rat and mouse tissue analysed. Rat mesangial cells synthesise gC1qBP, but do not express gC1qBP on the cell surface. In rat serum, gC1qBP is present at low levels.

Published

1997

191. Two parallel routes of the complement-mediated antibody-dependent enhancement of HIV-1 infection.

Author

Prohászka Z, Nemes J, Hidvégi T, Tóth FD, Kerekes K, Erdei A, Szabó J, Ujhelyi E, Thielens N, Dierich MP, Späth P, Ghebrehiwet B, Hampl H, Kiss J, Arlaud G, and Füst G

Subjects

Antibodies, Monoclonal immunology, Complement C1q pharmacology, Disease Progression, HIV Infections physiopathology, Humans, Tumor Cells, Cultured, Complement C1q immunology, HIV Antibodies immunology, HIV Envelope Protein gp41 immunology, HIV Infections immunology, HIV-1 immunology

Abstract

Objective: To study the mechanism of the complement-mediated antibody-dependent enhancement (C'-ADE) of HIV infection which may play a significant role in the progression of HIV-disease., Methods: In vitro complement activating and complement-mediated HIV-infection enhancing abilities of three human anti-gp41 monoclonal antibodies (MAb) were tested. C'-ADE was estimated using HIV-1IIIB and CR2 (CD21)-carrying MT-4 target cells. Normal human serum (NHS), purified C1q, C1q-deficient (C1qD) and C2-deficient (C2D) human sera were applied as complement sources., Results: All MAb mediated increased C1q binding to solid-phase gp41. All MAb had a marked dose-dependent and strictly complement-mediated HIV-infection enhancing effect. Mixtures of the MAb with purified C1q also significantly increased HIV-1 infection. C1qD serum had a markedly lower enhancing effect than NHS, which could be raised to normal level by addition of purified C1q. Pretreatment of the target cells with anti-CR2 antibodies only partially inhibited the enhancing effect of the MAb plus normal human serum., Conclusion: These novel findings indicate that besides the well-known facilitation of entry of HIV-1 by the interaction between virus-bound C3 fragments and CR2 present on the target cells, fixation of C1q to intact virions also results in an enhanced productive HIV-1 infection in the MT-4 cell cultures.

Published

1997

192. The C1q-binding cell membrane proteins cC1q-R and gC1q-R are released from activated cells: subcellular distribution and immunochemical characterization.

Author

Peterson KL, Zhang W, Lu PD, Keilbaugh SA, Peerschke EI, and Ghebrehiwet B

Subjects

Amino Acid Sequence, Blotting, Western, Burkitt Lymphoma immunology, Burkitt Lymphoma metabolism, Carrier Proteins, Complement Activating Enzymes metabolism, Complement C1q antagonists & inhibitors, Extracellular Space chemistry, Extracellular Space metabolism, Hemolysis immunology, Humans, Lymphocytes chemistry, Membrane Proteins blood, Membrane Proteins chemistry, Mitochondrial Proteins, Molecular Sequence Data, Protein Binding immunology, Receptors, Complement blood, Receptors, Complement isolation & purification, Solubility, Subcellular Fractions chemistry, Subcellular Fractions metabolism, Tumor Cells, Cultured, Complement C1q metabolism, Hyaluronan Receptors, Lymphocyte Activation, Lymphocytes metabolism, Membrane Glycoproteins, Membrane Proteins pharmacokinetics, Receptors, Complement chemistry, Receptors, Complement metabolism

Abstract

Two types of widely coexpressed cell surface C1q-binding proteins (C1q-R): a 60-kDa calreticulin-homolog which binds to the collagen-like "stalk" of C1q and a 33-kDa protein with affinity for the globular "heads" of the molecule, have been described. In this report, we show that the two molecules are also secreted by Raji cells and peripheral blood lymphocytes and can be isolated in soluble form from serum-free culture supernatant by HPLC purification using a Mono-Q column. The two purified soluble proteins had immunochemical and physical characteristics similar to their membrane counterparts in that both bound to intact C1q and to their respective C1q ligands, cC1q and gC1q. In addition, N-terminal amino acid sequence analyses of the soluble cC1q-R and gC1q-R were found to be identical to the reported sequences of the respective membrane-isolated proteins. Ligand blot analyses using biotinylated membrane or soluble cC1q-R and gC1q-R showed that both bind to the denatured and nondenatured A-chain and moderately to the C-chain of C1q. Moreover, like their membrane counterparts, the soluble proteins were found to inhibit serum C1q hemolytic activity. Although cC1q-R was released when both peripheral blood lymphocytes and Raji cells were incubated in phosphate-buffered saline for 1 hr under tissue culture conditions, gC1q-R was releasable only from Raji cells, suggesting that perhaps activation or transformation leading to immortalization is required for gC1q-R release. Subcellular fractionation of Raji cells and analyses by enzyme-linked immunosorbent assay and Western blotting showed that the two molecules are present in the cytosolic fractions as well as on the membrane. The data suggest that soluble forms of both C1q-binding molecules are released from cells and that these molecules may play important roles in vivo as regulators of complement activation.

Published

1997

193. The intrinsic coagulation/kinin-forming cascade: assembly in plasma and cell surfaces in inflammation.

Author

Kaplan AP, Joseph K, Shibayama Y, Reddigari S, Ghebrehiwet B, and Silverberg M

Subjects

Angioedema blood, Animals, Blood Cells physiology, Blood Coagulation Factors physiology, Bradykinin biosynthesis, Bradykinin chemistry, Bradykinin physiology, Carrier Proteins, Endothelium, Vascular physiopathology, Enzyme Activation, Enzyme Precursors metabolism, Factor XII chemistry, Fibrinolysis, Humans, Hypersensitivity blood, Kininogens chemistry, Macromolecular Substances, Mitochondrial Proteins, Models, Molecular, Plasminogen physiology, Prekallikrein chemistry, Protein Conformation, Receptors, Complement physiology, Zinc physiology, Blood Coagulation physiology, Factor XII physiology, Hyaluronan Receptors, Inflammation blood, Kininogens physiology, Kinins blood, Membrane Glycoproteins, Prekallikrein physiology

Published

1997

194. Human C1q induces eosinophil migration.

Author

Kuna P, Iyer M, Peerschke EI, Kaplan AP, Reid KB, and Ghebrehiwet B

Subjects

Blood Proteins metabolism, Cell Movement drug effects, Cell Movement physiology, Cell Survival drug effects, Complement C1q physiology, Eosinophil Granule Proteins, Eosinophils immunology, Humans, In Vitro Techniques, Integrin beta1 metabolism, Interleukin-3 pharmacology, Interleukin-5 pharmacology, Macrophage-1 Antigen metabolism, Mitochondrial Proteins, Proteins antagonists & inhibitors, Proteins immunology, Proteins physiology, Receptors, Complement antagonists & inhibitors, Receptors, Complement immunology, Receptors, Complement physiology, Carrier Proteins, Complement C1q pharmacology, Eosinophils drug effects, Eosinophils physiology, Hyaluronan Receptors, Membrane Glycoproteins, Ribonucleases

Abstract

Eosinophils (Eo) play a significant role in allergic inflammation and the host's immunity to parasitic infections. Although the presence of C1q-binding cell surface molecule(s) (C1q-R) on Eo had been previously implicated by the ability of C1q to augment IgG-dependent, Eo-mediated killing of schistosomula, little is known about the structure or the function of this receptor. The present studies were therefore undertaken to immunochemically demonstrate and to examine the biology of Eo C1q-R. Eo were purified to homogeneity (>90%) and viability (>98%) from hypereosinophilic donors by Percoll density gradient. Western blot analysis using antibodies to cC1q-R and gC1q-R showed distinct bands corresponding to cC1q-R (60 kDa) and gC1q-R (33 kDa) when immunoblotted with their respective antibodies. The Eo C1q-R was tested for its ability to induce chemokinesis and/or chemotaxis as assessed by the modified Boyden microchamber assay utilizing 5-micrometer-pore polycarbonate membranes and using C1q, cC1q, or gC1q (10 micrograms/ml) as agonists. The known chemotactic factors C5a and RANTES (10(-8)M) were used as positive controls. The results showed that at this concentration, cC1q was most efficient in its ability to induce Eo migration (20 +/- SEM 12, n = 4) followed by C1q (107 +/- SEM 7, n=7) and gC1q (77 +/- SEM 10, n = 10). When checkerboard analysis was performed, the data indicated that the observed phenomenon was likely to be due largely to chemokinesis. As expected, C5a (145 +/- SEM 15, n = 7) and RANTES (145 +/- SEM 43, n = 7) were both chemotactic. Furthermore, incubation of Eo with 50 micrograms of either C1q, gC1q, or cC1q (1 hr, 37 degrees C) did not cause release of eosinophil cationic protein as measured by RIA, nor did it enhance the expression of CD11b or CD29 as assessed by FACS analysis. The data presented in this paper show that Eo express both cC1q-R and gC1q-R and may participate in Eo function by providing a primary signal for locomotion.

Published

1996

195. Identification of functional domains on gC1Q-R, a cell surface protein that binds to the globular "heads" of C1Q, using monoclonal antibodies and synthetic peptides.

Author

Ghebrehiwet B, Lu PD, Zhang W, Lim BL, Eggleton P, Leigh LE, Reid KB, and Peerschke EI

Subjects

Amino Acid Sequence, Animals, Carrier Proteins, Humans, Membrane Proteins immunology, Membrane Proteins metabolism, Mice, Mice, Inbred BALB C, Mitochondrial Proteins, Molecular Sequence Data, Peptides immunology, Peptides metabolism, Protein Binding immunology, Receptors, Complement chemistry, Tumor Cells, Cultured, Antibodies, Monoclonal chemistry, Complement C1q metabolism, Hyaluronan Receptors, Membrane Glycoproteins, Peptides chemical synthesis, Receptors, Complement isolation & purification, Receptors, Complement physiology

Abstract

A membrane protein (33 kDa) that binds to the globular "heads" of C1q (gC1q-R) has been recently described. The full length cDNA encoding gC1q-R has been cloned, expressed in E. coli and using the purified recombinant protein (rgC1q-R) as an immunogen, a panel of IgG monoclonal antibodies (MAb) has been produced by fusion of spleen cells from hyperimmunized BALB/c mice with NSO mouse myeloma partners. From this fusion, 60 anti-gC1q-R hybridomas were selected and evaluated for their ability to (1) discriminate between the mature form (MF) of gC1q-R (residues 74-282) and a truncated form (TF) lacking residues 74-95, which contains a major C1q binding site, (2) recognize two functionally defined synthetic peptides derived from the NH2-(XN18) and COOH-(XC15) terminus of gC1q-R, and (3) bind to microtiter well fixed intact Raji cells. Several clones were identified: MAbs 46.23 and 60.11 (IgG1 kappa), reacted strongly with ELISA plate-fixed intact Raji and K562 cells, MF, and the XN18 peptide, but had poor or no reactivity with TF; MAbs 74.5.2 > 25.15 (IgG1 kappa) recognized both MF and TF and are directed against epitopes in the XC15 peptide that contains a binding site for high-molecular-weight kininogen and Factor XII.

Published

1996

196. Platelet membrane receptors for the complement component C1q.

Author

Peerschke EI and Ghebrehiwet B

Subjects

Amino Acid Sequence, Animals, Carrier Proteins, Complement C1q chemistry, Complement C1q metabolism, Humans, Mitochondrial Proteins, Molecular Sequence Data, Receptors, Complement chemistry, Blood Platelets physiology, Cell Membrane physiology, Hyaluronan Receptors, Membrane Glycoproteins, Receptors, Complement physiology

Published

1994

197. C1q inhibitor (chondroitin-4-sulfate proteoglycan): structure and function.

Author

Ghebrehiwet B and Galanakis DK

Subjects

Chondroitin Sulfate Proteoglycans isolation & purification, Chromatography, Affinity, Complement C1 Inactivator Proteins chemistry, Complement C1 Inactivator Proteins isolation & purification, Humans, Kinetics, Molecular Weight, Chondroitin Sulfate Proteoglycans chemistry, Chondroitin Sulfate Proteoglycans metabolism, Complement Activation, Complement C1 Inactivator Proteins metabolism, Complement C1q metabolism

Abstract

The serum C1q inhibitor (C1q INH) is a chondroitin 4-sulfate proteoglycan which is composed of several polyanionic components ranging in size from 21-750 kDa. Although the activity of C1q INH has been described in terms of its ability to precipitate C1q and inhibit its hemolytic activity, not much is known about either the mechanisms of its action or its role in health and disease. This report provides evidence that a 30 kDa core protein component of the proteoglycan macromolecule contains most of the C1q inhibitory activity. This inhibitory activity occurs as a result of C1q INH binding to the C1q "heads" (gC1q) as well as to the collagen "tail" (cC1q). What may be more significant in terms of perpetuation of inflammatory processes is the ability of C1q INH to moderately activate the classical pathway leading to C2 and C4 consumption. The binding of C1q INH to C1q is enhanced at low ionic strength, but significant binding does occur under physiologic conditions which makes it likely for the inhibitor to participate in inflammatory processes especially in microenvironments of high inhibitor concentration. Such elevated concentration does occur in patients with active rheumatoid arthritis and systemic lupus erythematosus either as a result of unregulated proteoglycan synthesis or disturbances in connective tissue metabolism. Another important function of serum C1q INH is its ability to prolong the clotting time of plasma and fibrinogen solutions containing or lacking CaCl2. This potent anticoagulant activity is again displayed by the 30 kDa putative protein core which specifically binds to both the E and D domains of fibrinogen. However, the epitope(s) on the 30 kDa which binds to C1q appears to be distinct from that which binds to fibrinogen. The known presence of proteoglycans on the basement membranes and other sites may explain at least in part the presence of fibrinogen in atheromatous lesions. Furthermore, by binding to fibrinogen, soluble C1q INH-and C1q-C1q INH complexes may limit fibrin gelation in inflammatory and tissue repair microenvironments.

Published

1993

198. The C1q-R participates in immunoregulation and signal transduction.

Author

Ghebrehiwet B and Peerschke EI

Subjects

Carrier Proteins, Cell Division, Humans, Mitochondrial Proteins, Receptors, Complement metabolism, Signal Transduction, Cell Adhesion, Complement C1q metabolism, Hyaluronan Receptors, Immunity, Membrane Glycoproteins, Receptors, Complement physiology

Abstract

The receptor for human C1q which recognizes the "collagen like" tail of its ligand is expressed on a wide range of cells including those which are not involved in the immune response. Nevertheless, the interaction of C1q with its receptor triggers a variety of cellular responses and these responses are suspected to involve certain signalling pathways. The few examples cited in this report provide ample evidence to support the long held notion that the cellular responses induced by C1q-C1q-R interaction involve signal transduction pathways. Platelets, for instance, can be activated by aggregated C1q. This activation, which is accompanied by a significant increase in the release of inositol-1,4,5-triphosphate (IP3) results in the expression of alpha 11b/beta 3 integrins (GPIIb/IIIa) and procoagulant activity and may contribute to thrombotic and inflammatory reactions. The ability of C1q to induce proliferative or anti-proliferative responses depend upon the nature of the C1q or the state of the cell expressing the C1q-R. In any event, even these responses most likely involve activation of transmembrane signal transduction pathway(s) which are yet to be elucidated.

Published

1993

199. Isolation of a human endothelial cell C1q receptor (C1qR).

Author

Peerschke EI, Malhotra R, Ghebrehiwet B, Reid KB, Willis AC, and Sim RB

Subjects

Amino Acid Sequence, Autoradiography, Carrier Proteins, Cells, Cultured, Chromatography, High Pressure Liquid, Chromatography, Ion Exchange, Humans, Iodine Radioisotopes, Kinetics, Mitochondrial Proteins, Molecular Sequence Data, Molecular Weight, Receptors, Complement metabolism, Umbilical Veins, Endothelium, Vascular immunology, Hyaluronan Receptors, Membrane Glycoproteins, Receptors, Complement isolation & purification

Abstract

C1q binding to endothelial cells has been described previously, but the putative cell surface receptor(s) has not been identified. In the present study, modifications of a reported purification of lymphocyte C1q receptor (C1qR) were used to isolate C1q binding sites from human umbilical vein endothelial cells. Cells were harvested, without protease treatment, at passage 10-17 and lysed with 1% Triton X-100. The lysate was fractionated on Fast-performance liquid chromatography (FPLC) Mono-Q using a linear NaCl gradient, followed by high-performance liquid chromatography (HPLC) ion exchange (TSKgel DEAE-NPR). A major protein was eluted that had the same mobility on sodium dodecyl sulfate-polyacrylamide gels and the same NH2-terminal sequence as lymphocyte C1qR. This protein was expressed on the surface, as judged by surface radioiodination, bound to C1q-coated surfaces, and was recognized by polyclonal antilymphocyte C1qR antibodies. Thus, endothelial cells express a C1q receptor that appears identical to lymphocyte C1qR. The data further support the hypothesis that cell surface C1qRs identified on a variety of somatic and cultured cells are either identical or constitute a family of closely related molecules.

Published

1993

200. Short amino acid sequences derived from C1q receptor (C1q-R) show homology with the alpha chains of fibronectin and vitronectin receptors and collagen type IV.

Author

Ghebrehiwet B, Peerschke EI, Hong Y, Munoz P, and Gorevic PD

Subjects

Amino Acid Sequence, Amino Acids analysis, Carrier Proteins, Collagen metabolism, Humans, Mitochondrial Proteins, Molecular Sequence Data, Receptors, Complement analysis, Receptors, Complement metabolism, Receptors, Fibronectin, Receptors, Vitronectin, Collagen chemistry, Complement Activating Enzymes metabolism, Fibronectins metabolism, Hyaluronan Receptors, Integrins metabolism, Membrane Glycoproteins, Receptors, Complement chemistry, Receptors, Immunologic chemistry

Abstract

The human C1q receptor (C1q-R) is a 65-70-kd, highly acidic, hydrophobic glycoprotein that is expressed on a wide variety of cell surfaces. Although the C1q-R itself appears to bind preferentially to C1q, the region of the ligand to which C1q-R binds is the primary binding site for several other molecules, including fibronectin, laminin, and C1q inhibitor (chondroitin 4-sulfate proteoglycan) as well as the complement C1r2C1s2 tetramer. In order to further characterize the C1q-R molecule with regard to its structure and function, highly purified C1q-R was obtained from Raji cells using DEAE-Sephacel and C1q-Sepharose CL-4B chromatography. Studies performed with 125I-labeled C1q-R demonstrated that whereas the C1q-R molecule binds poorly to a variety of human collagens including types II, III, and V, markedly enhanced binding is observed with type IV collagen and moderately enhanced binding with type I collagen. Amino acid composition studies show that the C1q-R molecule contains approximately 44% hydrophobic and 12.6% hydrophilic residues with a ratio of negatively charged to positively charged residues of about 2:1. Treatment of 125I-labeled C1q-R with endoglycosidase F lowers the apparent molecular size from 70 to 58 kd, whereas endoglycosidase H lowered the size to 64 kd. Treatment with neuraminidase, on the other hand, shifted the size of C1q-R to 60 kd. These results suggest the presence of several highly sialylated complex-type or high mannose-type N-linked oligosaccharide side chains. Because purified C1q-R has a blocked amino terminus, amino acid sequences representing internal fragments of the molecule were generated by electroblotting and in situ enzymatic digestion. When these short sequences were searched against the National Biomedical Research Foundation computer data base, a seven-amino-acid sequence, VSWQGQI, showed significant homology (100% and 80% in a five-amino-acid overlap, respectively) with the alpha chains of the human fibronectin (alpha 5 beta 1) and vitronectin (alpha v beta 3) receptors, and to a lesser degree with epidermal growth factor receptor and T cell receptor. A second sequence, ISEDNIR, showed homology with mouse collagen type IV (86% in a six-amino-acid overlap), calmodulin (60% in a seven-amino-acid overlap), and a Leishmania major surface antigen, gp63. These observations seem to predict that C1q-R has pockets of conserved sequences that are similar to those not only present in its ligand(s) but also in other cell surface receptors that may, in part, fulfill similar functions.

Published

1992