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1. Gene Expression and Function of the Cellular Receptor for u-PA (u-PAR)

Author

Torben Plesner, Michael Ploug, Keld Dano, and Vincent Ellis

Subjects
Proteases, Chemistry, Growth factor, medicine.medical_treatment, Cell, Tissue plasminogen activator, Cell biology, Serine, medicine.anatomical_structure, Gene expression, medicine, Plasminogen activator, Function (biology), medicine.drug
Abstract

Plasminogen activation, catalyzed by the serine proteases urokinase-type plasminogen activator (u-PA) and tissue plasminogen activator (t-PA), is thought to play an important role in a variety of physiological and pathological processes. The potency of the plasminogen activation system indicates that specific mechanisms must exist to control the initiation, progression, localization, and termination of the system. The principal role of u-PAR is to provide a facile mechanism for the confinement of u-PA to the cell surface, and this is accomplished by the high-affinity interaction between the growth factor domain of u-PA and the amino-terminal domain of u-PAR. The explanation for the discrepancy in the effects of u-PAR in purified and cell-associated systems lies in the binding of plasminogen to the cell surface. The cellular potentiation of plasminogen activation has been shown to involve effects on the activation of both plasminogen and pro-u-PA, which together account for the overall effect.

Published
2019

2. Modulation of the urokinase-type plasminogen activator receptor by the β6 integrin subunit

Author

Rosemary Bass, Vincent Ellis, Simon A. Whawell, Mark R. Morgan, John Marshall, Gareth J. Thomas, Paul M. Speight, and Nafisa Dalvi

Subjects
Keratinocytes, Integrin beta Chains, Integrin, Biophysics, Receptors, Cell Surface, Biochemistry, CD49c, Receptors, Urokinase Plasminogen Activator, Cell Movement, Tumor Cells, Cultured, medicine, Humans, Fibrinolysin, RNA, Messenger, Receptor, Melanoma, Molecular Biology, Urokinase, Mouth, biology, Cell Membrane, Cell Biology, Flow Cytometry, Urokinase-Type Plasminogen Activator, Molecular biology, Fibronectins, Cell biology, Urokinase receptor, Integrin alpha M, Carcinoma, Squamous Cell, biology.protein, Mouth Neoplasms, Integrin, beta 6, Plasminogen activator, medicine.drug
Abstract

Over-expression of components of the urokinase system is well documented in cancer and is thought to enable tumour cells to migrate and invade. Changes in integrin expression are also a common feature of tumours and have been linked to changes in protease activity. It has been shown that the alphavbeta6 integrin is neo-expressed in a number of epithelial carcinomas and in wound healing situations. We therefore investigated whether alphavbeta6 is able to modulate a key regulator of proteolysis, the urokinase receptor. We report that epithelial cells expressing full-length alphavbeta6 exhibit decreased urokinase receptor expression and function. Furthermore, this novel modulation requires the C-terminal 11 amino acids of the cytoplasmic tail of the beta6 integrin subunit. Cells expressing alphavbeta3, however, did not affect urokinase receptor expression. De novo expression of beta6 by melanoma cells and beta3 by epithelial cells did not influence urokinase receptor expression or function, suggesting that modulation of urokinase system is both integrin subunit and cell-specific.

Published
2004

3. Plasminogen Activation Is Stimulated by Prion Protein and Regulated in a Copper-Dependent Manner

Author

Vincent Ellis, Rashmi Misra, David R. Brown, and Maki Daniels

Subjects
PrPSc Proteins, Prions, animal diseases, Plasma protein binding, Biochemistry, Tissue plasminogen activator, Prion Diseases, law.invention, Mice, Enzyme activator, law, Zymogen, medicine, Animals, PrPC Proteins, Binding site, Serine protease, biology, Plasminogen, Urokinase-Type Plasminogen Activator, Molecular biology, Recombinant Proteins, nervous system diseases, Enzyme Activation, Tissue Plasminogen Activator, biology.protein, Recombinant DNA, Apoproteins, Copper, Protein Binding, medicine.drug
Abstract

Prion diseases are associated with the conversion of the normal prion protein, PrP(C), to the infectious disease form PrP(Sc). Discrimination between these isoforms would significantly enhance diagnosis of these diseases, and it has recently been reported that PrP(Sc) is specifically recognized by the serine protease zymogen plasminogen (Fischer et al. (2000) Nature 408, 479). Here we have tested the hypothesis that PrP is a regulator of the plasminogen activation system. The effect of recombinant PrP, either containing copper (holo-PrP) or devoid of it (apo-PrP), on plasminogen activation by both uPA and tPA was determined. PrP had no effect on plasminogen activation by uPA. By contrast, the activity of tPA was stimulated by up to 280-fold. This was observed only with the apo-PrP isoforms. The copper-binding octapeptide repeat region of PrP was involved in the effects, as a mutant lacking this region failed to stimulate plasminogen activation, although a synthetic peptide corresponding to this region was unable to stimulate tPA activity. Competition experiments demonstrated that, in addition to plasminogen binding, the stimulation required a high-affinity interaction between tPA and PrP (K(d) < 2.5 nM). Kinetic analysis revealed a template mechanism for the stimulation, suggesting independent binding sites for tPA and plasminogen. Lack of copper-binding may be an early event in the conversion of PrP(C) to PrP(Sc), and our data therefore suggest that tPA-catalyzed plasminogen activation may provide the basis for a sensitive detection system for the early stages of prion diseases and also play a role in the pathogenesis of these diseases.

Published
2002

4. Cellular mechanisms regulating non-haemostatic plasmin generation

Author

Vincent Ellis and Rosemary Bass

Subjects
Proteases, Plasmin, Receptors, Cell Surface, Serpin, Biology, Models, Biological, Biochemistry, Tissue plasminogen activator, Muscle, Smooth, Vascular, Receptors, Urokinase Plasminogen Activator, Extracellular matrix, Mice, medicine, Animals, Humans, Fibrinolysin, Hemostasis, Membrane Proteins, Neurodegenerative Diseases, Plasminogen, Cell migration, Urokinase-Type Plasminogen Activator, Urokinase receptor, Plasminogen activator, medicine.drug
Abstract

A variety of proteases have the potential to degrade the extracellular matrix (ECM), thereby influencing the behaviour of cells by removing physical barriers to cell migration, altering cell-ECM interactions or releasing ECM-associated growth factors. The plasminogen activation system of serine proteases is particularly implicated in this pericellular proteolysis and is involved in pathologies ranging from cancer invasion and metastasis to fibroproliferative vascular disorders and neurodegeneration. A central mechanism for regulating plasmin generation is through the binding of the two plasminogen activators to specific cellular receptors: urokinase-type plasminogen activator to the glycolipid-anchored membrane protein uPAR, and tissue plasminogen activator to a type-II transmembrane protein recently identified on vascular smooth muscle cells. These binary complexes interact with membrane-associated plasminogen to form higher order activation complexes that greatly reduce the Km for plasminogen activation and, in some cases, protect the proteases from their cognate serpin inhibitors. Various other proteins that are involved in cell adhesion and migration also interact with these complexes, modulating the activity of this efficient and spatially restricted proteolytic system. Recent observations demonstrate that certain forms of the prion protein can stimulate tissue plasminogen activator-catalysed plasminogen activation, which raises the possibility that these proteases may also have a role in the pathogenesis of the transmissible spongiform encephalopathies.

Published
2002

5. Receptor-mediated regulation of plasminogen activator function: plasminogen activation by two directly membrane-anchored forms of urokinase

Author

David J. Vines, Vincent Ellis, Sung W. Lee, and David A. Dichek

Subjects
Pharmacology, Urokinase, Serine protease, biology, Chemistry, Plasmin, Organic Chemistry, General Medicine, Receptor-mediated endocytosis, Biochemistry, Urokinase receptor, Structural Biology, Zymogen, Drug Discovery, medicine, biology.protein, Molecular Medicine, Receptor, Molecular Biology, Plasminogen activator, medicine.drug
Abstract

The generation of the broad specificity serine protease plasmin in the pericellular environment is regulated by binding of the urokinase-type plasminogen activator (uPA) to its specific glycosylphosphatidylinositol (GPI)-anchored cell-surface receptor, uPAR. This interaction potentiates the reciprocal activation of the cell-associated zymogens pro-uPA and plasminogen. To further study the role of uPAR in this mechanism, we have expressed two directly membrane-anchored chimeric forms of uPA, one anchored by a C-terminal GPI-moiety (GPI-uPA), the other with a C-terminal transmembrane peptide (TM-uPA). These were expressed in the monocyte-like cell lines U937 and THP-1, which are excellent models for kinetic and mechanistic studies of cell-surface plasminogen activation. In both cell-lines, GPI-uPA activated cell-associated plasminogen with characteristics both qualitatively and quantitatively indistinguishable from those of uPAR-bound uPA. By contrast, TM-uPA activated cell-associated plasminogen less efficiently. This was due to effects on the Km for plasminogen activation (which was increased up to five-fold) and the efficiency of pro-uPA activation (which was decreased approximately four-fold). These observations suggest that uPAR serves two essential roles in mediating efficient cell-surface plasminogen activation. In addition to confining uPA to the cell-surface, the GPI-anchor plays an important role by increasing accessibility to substrate plasminogen and, thus, enhancing catalysis. However, the data also demonstrate that, in the presence of an alternative mechanism for uPA localization, uPAR is dispensable and, therefore, unlikely to participate in any additional interactions that may be necessary for the efficiency of this proteolytic system. In these experiments zymogen pro-uPA was unexpectedly found to be constitutively activated when expressed in THP-1 cells, suggesting the presence of an alternative plasmin-independent proteolytic activation mechanism in these cells. Copyright © 2000 European Peptide Society and John Wiley & Sons, Ltd.

Published
2000

6. Tissue Plasminogen Activator Binds to Human Vascular Smooth Muscle Cells by a Novel Mechanism

Author

Vincent Ellis, Finn Werner, and Tahir M. Razzaq

Subjects
Serine protease, Circular dichroism, Vascular smooth muscle, integumentary system, biology, Activator (genetics), Cell Biology, Biochemistry, Tissue plasminogen activator, chemistry.chemical_compound, Protein structure, chemistry, Plasminogen activator inhibitor-1, Biophysics, biology.protein, medicine, Binding site, Molecular Biology, medicine.drug
Abstract

Human vascular smooth muscle cells (VSMC) bind tissue plasminogen activator (tPA) specifically, saturably, and with relatively high affinity (K(d) 25 nM), and this binding potentiates the activation of cell-associated plasminogen (Ellis, V., and Whawell, S. A. (1997) Blood 90, 2312-2322). We have observed that this binding can be efficiently competed by DFP-inactivated tPA and S478A-tPA but not by tPA inactivated with H-D-Phe-Pro-Arg-chloromethyl ketone (PPACK). VSMC-bound tPA also exhibited a markedly reduced inhibition by PPACK, displaying biphasic kinetics with second-order rate constants of 7. 5 x 10(3) M(-1) s(-1) and 0.48 x 10(3) M(-1) s(-1), compared with 7. 2 x 10(3) M(-1) s(-1) in the solution phase. By contrast, tPA binding to fibrin was competed equally well by all forms of tPA, and its inhibition was unaltered. These effects were shown to extend to the physiological tPA inhibitor, plasminogen activator inhibitor 1. tPA.plasminogen activator inhibitor 1 complex did not compete tPA binding to VSMC, and the inhibition of bound tPA was reduced by 30-fold. The behavior of the various forms of tPA bound to VSMC correlated with conformational changes in tPA detected by CD spectroscopy. These data suggest that tPA binds to its specific high affinity site on VSMC by a novel mechanism involving the serine protease domain of tPA and distinct from its binding to fibrin. Furthermore, reciprocally linked conformational changes in tPA appear to have functionally significant effects on both the interaction of tPA with its VSMC binding site and the susceptibility of bound tPA to inhibition.

Published
1999

7. Vascular Smooth Muscle Cells Potentiate Plasmin Generation by Both Urokinase and Tissue Plasminogen Activator-Dependent Mechanisms: Evidence for a Specific Tissue-Type Plasminogen Activator Receptor on These Cells

Author

Vincent Ellis and Simon A. Whawell

Subjects
Urokinase, medicine.medical_specialty, Vascular smooth muscle, T-plasminogen activator, Plasmin, Immunology, Cell Biology, Hematology, Biology, Biochemistry, Tissue plasminogen activator, Cell biology, Urokinase receptor, Endocrinology, Internal medicine, medicine, Binding site, Plasminogen activator, medicine.drug
Abstract

Plasminogen activators play a role in the response of the vessel wall to injury, presumably by mediating the degradation of extracellular matrix (ECM) by vascular smooth muscle cells (VSMCs) that is necessary for their migration and proliferation. We have therefore investigated the ability of VSMCs to assemble specific cell surface plasminogen-activating systems. Urokinase-type plasminogen activator (uPA) bound to a single class of site on VSMCs (kd, 2 nmol/L), binding of pro-uPA resulted in a large potentiation of plasmin generation and both were competed by antibodies to the uPA receptor (uPAR). Tissue-type plasminogen activator (tPA) also bound to VSMCs as determined by functional assay, with the binding isotherms showing two classes of binding site with apparent kds of 25 and 300 nmol/L. tPA binding to the higher affinity site caused a greater than 90-fold enhancement of the activation of cell bound plasminogen, whereas the lower affinity binding, mediated primarily by the ECM, had little effect on tPA activity. The high-affinity binding of tPA to VSMCs resulted in an eightfold greater potential for plasmin generation than the binding of uPA, with this difference increasing to 15-fold after thrombin stimulation of the cells due to a 1.8-fold increase in tPA binding. These data show a novel specific tPA receptor on VSMCs that may be important for the regulation of plasminogen activation in various vascular pathologies.

Published
1997

8. Potent and specific inhibition of the biological activity of the type-II transmembrane serine protease matriptase by the cyclic microprotein MCoTI-II

Author

Kelly Gray, Vincent Ellis, Kate A. Owen, Panumart Thongyoo, Thomas H. Bugge, Salma Elghadban, Roman Szabo, Edward W. Tate, and Robin J. Leatherbarrow

Subjects
0301 basic medicine, Male, cyclotide, Time Factors, medicine.medical_treatment, HEPATOCYTE GROWTH-FACTOR, Cyclotides, matriptase, Madin Darby Canine Kidney Cells, Substrate Specificity, 0302 clinical medicine, Cell Movement, Electric Impedance, Molecular Targeted Therapy, AFFINITY, PERIPHERAL VASCULAR DISEASE, biology, Hepatocyte Growth Factor, CARCINOGENESIS, Serine Endopeptidases, Hematology, CANCER, Transmembrane protein, Serine protease, Biochemistry, 030220 oncology & carcinogenesis, Hepatocyte growth factor, Life Sciences & Biomedicine, medicine.drug, Proteases, Serine Proteinase Inhibitors, SURFACE, Hepsin, Transfection, Tight Junctions, protease inhibitor, 03 medical and health sciences, EPIDERMAL DIFFERENTIATION, Dogs, Cell Line, Tumor, medicine, Animals, Humans, Matriptase, Neoplasm Invasiveness, PLASMINOGEN-ACTIVATOR, Protein Precursors, Protease, Science & Technology, epithelial cell, Prostatic Neoplasms, 030104 developmental biology, HEK293 Cells, Zymogen activation, ZYMOGEN ACTIVATION, biology.protein, Cardiovascular System & Cardiology, FACTOR ACTIVATOR INHIBITOR-1, PROSTASIN PROTEOLYTIC CASCADE
Abstract

SummaryMatriptase is a type-II transmembrane serine protease involved in epithelial homeostasis in both health and disease, and is implicated in the development and progression of a variety of cancers. Matriptase mediates its biological effects both via as yet undefined substrates and pathways, and also by proteolytic cleavage of a variety of well-defined protein substrates, several of which it shares with the closely-related protease hepsin. Development of targeted therapeutic strategies will require discrimination between these proteases. Here we have investigated cyclic microproteins of the squash Momordica cochinchinensis trypsin-inhibitor family (generated by total chemical synthesis) and found MCoTI-II to be a high-affinity (Ki 9 nM) and highly selective (> 1,000-fold) inhibitor of matriptase. MCoTI-II efficiently inhibited the proteolytic activation of pro-hepatocyte growth factor (HGF) by matriptase but not by hepsin, in both purified and cell-based systems, and inhibited HGF-dependent cell scattering. MCoTI-II also selectively inhibited the invasion of matriptase-expressing prostate cancer cells. Using a model of epithelial cell tight junction assembly, we also found that MCoTI-II could effectively inhibit the re-establishment of tight junctions and epithelial barrier function in MDCK-I cells after disruption, consistent with the role of matriptase in regulating epithelial integrity. Surprisingly, MCoTI-II was unable to inhibit matriptase-dependent proteolytic activation of prostasin, a GPI-anchored serine protease also implicated in epithelial homeostasis. These observations suggest that the unusually high selectivity afforded by MCoTI-II and its biological effectiveness might represent a useful starting point for the development of therapeutic inhibitors, and further highlight the role of matriptase in epithelial maintenance.

Published
2013

9. u-Plasminogen Activator

Author

Vincent Ellis

Subjects
Proteases, Materials science, Protease, biology, Activator (genetics), Plasmin, Chemistry, medicine.medical_treatment, Cleavage (embryo), Molecular biology, Fibrin, Biochemistry, U-plasminogen activator, Fibrinolysis, medicine, biology.protein, medicine.drug
Abstract

u-Plasminogen activator (uPA) is one of two highly specific mammalian proteases responsible for the activation of plasminogen by specific cleavage of an Arg-Val bond to form the broad substrate specificity protease plasmin. This activity gives it a central role both in the haemostatic process (via the dissolution of fibrin = fibrinolysis) and in the generation of pericellular proteolytic activity, which is implicated in many pathologies involving tissue remodeling/degradation …

Published
2013

10. Functional Analysis of the Cellular Receptor for Urokinase in Plasminogen Activation

Author

Vincent Ellis

Subjects
Urokinase, Protease, Intrinsic activity, Plasmin, Chemistry, medicine.medical_treatment, Cell Biology, Biochemistry, biological factors, Urokinase receptor, enzymes and coenzymes (carbohydrates), Zymogen activation, medicine, Binding site, skin and connective tissue diseases, neoplasms, Molecular Biology, Plasminogen activator, medicine.drug
Abstract

Plasminogen activation catalyzed by the urokinase-type plasminogen activator (uPA) constitutes a reciprocal zymogen activation system, as plasmin can efficiently activate pro-uPA, the single-chain zymogenic form of the protease. We have previously shown that the overall efficiency of this plasminogen activation system is greatly enhanced by its assembly on the cell surface, involving binding of pro-uPA to its cellular binding site uPAR, and the concurrent cellular binding of plasminogen. We have now studied the effect of a recombinant soluble form of uPAR (residues 1–277) on the proteolytic reactions of this system. In contrast to the increased efficiencies of plasminogen activation and pro-uPA activation observed with cell-surface uPAR, soluble uPAR had an inhibitory effect on both of these individual reactions. Soluble uPAR also caused no increase in the low, but discernible, intrinsic activity of pro-uPA. Consistent with the observations on the isolated reactions, the overall activity of the pro-uPA-mediated plasminogen activation system was significantly inhibited. These observations confirm the previous interpretation of the observations made with cell-surface uPAR that the mechanism of the enhanced plasmin generation is due to the catalytically favorable interaction of uPAR-bound uPA/pro-uPA with cell-bound plasminogen/plasmin, rather than direct effects on the properties of uPA or pro-uPA on binding to uPAR.

Published
1996

11. Structure-function relationships in the receptor for urokinase-type plasminogen activator Comparison to other members of the Ly-6 family and snake venom α-neurotoxins

Author

Michael Ploug and Vincent Ellis

Subjects
Molecular Sequence Data, Neurotoxins, Biophysics, CD59, Bungarotoxin, Biochemistry, Structure-Activity Relationship, Structural Biology, Cell surface receptor, Genetics, medicine, Animals, Antigens, Ly, uPA, Amino Acid Sequence, skin and connective tissue diseases, neoplasms, Molecular Biology, Urokinase, Chemistry, MIRL, Glycosyl-phosphatidylinositol, Cell Biology, Urokinase-Type Plasminogen Activator, biological factors, Cell biology, Urokinase receptor, enzymes and coenzymes (carbohydrates), Membrane protein, Snake venom, biological phenomena, cell phenomena, and immunity, uPAR, Plasminogen activator, medicine.drug
Abstract

Plasminogen activation is regulated by the interaction between urokinase-type plasminogen activator (uPA) and its specific glycolipid-anchored cell surface receptor (uPAR). uPAR is composed of three homologous domains and is the only multi-domain member of the Ly-6 family of glycolipid-anchored membrane proteins. Recent evidence has highlighted similarities between the individual domains of uPAR and the large family of secreted, single domain snake venom alpha-neurotoxins, suggesting that uPAR may adopt the same gross folding pattern as these structurally well characterized proteins. Structural aspects of the binding between alpha-neurotoxins and the acetylcholine receptor may have a major influence on future studies of the interaction between uPA and uPAR.

Published
1994

12. Urokinase plasminogen activator cleaves its cell surface receptor releasing the ligand-binding domain

Author

Gunilla Høyer-Hansen, Niels Behrendt, Michael Ploug, Keld Danø, Leif R. Lund, Helene Solberg, Ebbe Rønne, and Vincent Ellis

Subjects
Plasmin, Blotting, Western, Receptors, Cell Surface, Biology, Ligands, Biochemistry, Cell Line, Receptors, Urokinase Plasminogen Activator, Aprotinin, Cell surface receptor, medicine, Humans, Trypsin, Fibrinolysin, Binding site, Receptor, Molecular Biology, Urokinase, Binding Sites, Binding protein, Antibodies, Monoclonal, Cell Biology, Urokinase-Type Plasminogen Activator, Molecular biology, biological factors, Urokinase receptor, Kinetics, Tetradecanoylphorbol Acetate, Electrophoresis, Polyacrylamide Gel, Lymphoma, Large B-Cell, Diffuse, Plasminogen activator, medicine.drug
Abstract

The cellular receptor for urokinase-type plasminogen activator (uPAR) is a glycolipid-anchored three-domain membrane protein playing a central role in pericellular plasminogen activation. We have found that urokinase (uPA) can cleave its receptor between domains 1 and 2 generating a cell-associated uPAR variant without ligand-binding properties. In extracts of U937 cells there are two uPAR variants which after complete deglycosylation have apparent molecular masses of 35,000 and 27,000. Analysis with monoclonal antibodies showed that these variants represented the intact uPAR and a two-domain form, uPAR(2+3), lacking ligand-binding domain 1. Trypsin treatment showed that both variants are present on the outside of the cells. Addition to the culture medium of an anticatalytic monoclonal antibody to uPA inhibited the formation of the uPAR(2+3), indicating that uPA is involved in its generation. Purified uPAR can be cleaved directly by uPA as well as by plasmin. The uPA-catalyzed cleavage does not require binding of the protease to the receptor through its epidermal growth factor-like receptor-binding domain, since low molecular weight uPA that lacks this domain also cleaves uPAR. This unusual reaction in which a specific binding protein is proteolytically inactivated by its own ligand may represent a regulatory step in the plasminogen activation cascade.

Published
1992

13. Cell-induced potentiation of the plasminogen activation system is abolished by a monoclonal antibody that recognizes the NH2-terminal domain of the urokinase receptor

Author

Niels Behrendt, Gunilla Høyer-Hansen, Keld Danø, Michael Ploug, Ebbe Rønne, and Vincent Ellis

Subjects
Monoclonal antibody, medicine.drug_class, Plasmin, Biophysics, U937 cell, Receptors, Cell Surface, Biochemistry, Epitope, Cell Line, Receptors, Urokinase Plasminogen Activator, Epitopes, Plasminogen Activators, Structure-Activity Relationship, Structural Biology, Genetics, medicine, Chymotrypsin, Humans, Fibrinolysin, Molecular Biology, Urokinase, biology, Chemistry, Antibodies, Monoclonal, Plasminogen, Cell Biology, Precipitin Tests, Molecular biology, Urokinase receptor, Kinetics, biology.protein, Plasminogen activation, Antibody, Plasminogen activator, medicine.drug, Binding domain
Abstract

We have raised four monoclonal antibodies recognizing different epitopes within the human cell-surface receptor for urokinase-type plasminogen activator (u-PA). One of these antibodies completely abolishes the potentiation of plasmin generation observed upon incubation of the zymogens pro-u-PA and plasminogen with U937 cells. This antibody, which is also the only one to completely inhibit the binding of DFP-inactivated [125I]-u-PA to U937 cells, is directed against the u-PA binding NH2-terminal domain of u-PAR, a well-defined fragment formed by limited chymotrypsin digestion of purified u-PAR, demonstrating the functional independence of the u-PA binding domain as well as the critical role of u-PAR in the assembly of the cell-surface plasminogen activation system.

Published
1991

14. Plasminogen Activation by Receptor-Bound Urokinase

Author

Keld Danø and Vincent Ellis

Subjects
chemistry.chemical_classification, Urokinase, business.industry, Plasminogen, Receptors, Cell Surface, Hematology, Urokinase-Type Plasminogen Activator, Receptors, Urokinase Plasminogen Activator, Plasminogen Activators, Enzyme, Text mining, chemistry, Biochemistry, medicine, Humans, Protease Inhibitors, Cardiology and Cardiovascular Medicine, business, Receptor, medicine.drug
Published
1991

15. Activation of pro-BDNF by the pericellular serine protease plasmin

Author

Vincent Ellis and Kelly Gray

Subjects
Male, Proteases, animal structures, Neurite, Plasmin, viruses, Biophysics, PC12 Cells, Biochemistry, Structural Biology, Neurotrophic factors, Neurites, Genetics, medicine, Animals, Humans, Receptor, trkB, Fibrinolysin, Protein Precursors, Molecular Biology, Furin, Serine protease, Brain-derived neurotrophic factor, biology, Activator (genetics), Chemistry, Brain-Derived Neurotrophic Factor, Cell Membrane, Cell Biology, Proteolytic processing, Recombinant Proteins, Rats, BDNF, nervous system, embryonic structures, Mutagenesis, Site-Directed, biology.protein, Neurotrophin, medicine.drug
Abstract

Brain-derived neurotrophic factor (BDNF) is secreted as either a mature furin-processed form or an unprocessed pro-form. Here, we characterise the extracellular processing of pro-BDNF by the serine protease plasmin. Using recombinant BDNF, maintained in the pro-form by site-directed mutagenesis or inhibition of furin, we demonstrate that plasmin (but not related proteases) is a specific and efficient activator of pro-BDNF. The proteolytic cleavage site is identified as Arg125-Val, within the consensus furin-cleavage motif (RVRR), generating an active form that stimulated neurite outgrowth on TrkB-transfected PC12 cells. Furthermore, we demonstrate that this processing can also occur in the pericellular environment by the action of cell-associated plasminogen activators.

Published
2008

16. Inhibition of receptor-bound urokinase by plasminogen-activator inhibitors

Author

Niels Behrendt, Ebbe Rønne, T C Wun, Vincent Ellis, and Keld Danø

Subjects
Receptors, Cell Surface, Antigen-Antibody Complex, Biochemistry, Antibodies, Cell Line, Receptors, Urokinase Plasminogen Activator, Plasminogen Activators, chemistry.chemical_compound, Plasminogen Inactivators, Tumor Cells, Cultured, medicine, Humans, Binding site, Receptor, Molecular Biology, Urokinase, Enzyme Precursors, biology, Chemistry, Plasminogen, Cell Biology, Urokinase-Type Plasminogen Activator, Molecular biology, Urokinase receptor, Kinetics, biology.protein, Phorbol, Tetradecanoylphorbol Acetate, Vitronectin, Plasminogen activator, medicine.drug
Abstract

Urokinase-type plasminogen activator (uPA) binds to a specific receptor on various cell types, the bound molecule retaining its enzymatic activity against plasminogen. We have now investigated whether receptor-bound uPA also retains the ability to react with and be inhibited by plasminogen activator inhibitors (PAI-1 and PAI-2). uPA bound to its receptor on human U937 monocyte-like cells was inhibited by PAI-1 (in its active form in the presence of vitronectin fragments) with an association rate constant of 4.5 x 10(6) M-1 s-1, which was 40% lower than that obtained for uPA in solution (7.9 x 10(6) M-1 s-1). The inhibition of uPA by PAI-2 was decreased to a similar extent by receptor binding, falling from 5.3 x 10(5) to 3.3 x 10(5) M-1 s-1. Stimulation of U937 cells with phorbol 12-myristate 13-acetate was accompanied by a further reduction in receptor-bound uPA inhibition by PAI-1 and PAI-2 to 1.7 x 10(6) and 1.1 x 10(5) M-1 s-1, respectively. These constants although lower than those for uPA in solution still represent rather rapid inhibition of the enzyme, and demonstrate that uPA bound to its specific cellular receptor remains available for efficient inhibition by PAI's, which may therefore play a major role in controlling cell-surface plasminogen activation and extracellular proteolytic activity.

Published
1990

17. Functional regulation of tissue plasminogen activator on the surface of vascular smooth muscle cells by the type-II transmembrane protein p63 (CKAP4)

Author

David J. Vines, Tahir M. Razzaq, Vincent Ellis, Rosemary Bass, Finn Werner, and Simon A. Whawell

Subjects
Vascular smooth muscle, Endoplasmic Reticulum, Biochemistry, Tissue plasminogen activator, Mass Spectrometry, Muscle, Smooth, Vascular, Affinity chromatography, medicine, Animals, Humans, Binding site, Molecular Biology, Aorta, integumentary system, Chemistry, Endoplasmic reticulum, Antibodies, Monoclonal, Membrane Proteins, Plasminogen, Cell Biology, Molecular biology, Transmembrane protein, Rats, Blot, Tissue Plasminogen Activator, Mutation, Heterologous expression, medicine.drug, Protein Binding
Abstract

We have demonstrated that tissue plasminogen activator (tPA) binds specifically to human vascular smooth muscle cells (VSMC) in a functionally relevant manner, both increasing plasminogen activation and decreasing tPA inhibition (Ellis, V., and Whawell, S. A. (1997) Blood 90, 2312-2322; Werner, F., Razzaq, T. M., and Ellis, V. (1999) J. Biol. Chem. 274, 21555-21561). To further understand this system we have now identified and characterized the protein responsible for this binding. Rat VSMC were surface-labeled with 125I, and cell lysates were subjected to an affinity chromatography scheme based on the previously identified tPA binding characteristics. A single radiolabeled protein of 63 kDa bound specifically and was eluted at low pH. This protein was isolated from large scale preparations of VSMC and unambiguously identified as the rat homologue of the human type-II transmembrane protein p63 (CKAP4) by matrix-assisted laser desorption ionization and nano-electrospray tandem mass spectrometry of tryptic fragments. In confirmation of this, a monoclonal antibody raised against authentic human p63 recognized the isolated protein in Western blotting. Immunofluorescence microscopy demonstrated that p63 was located principally in the endoplasmic reticulum but was also detected in significant quantities on the surface of human VSMC. In support of the hypothesis that p63 is the functional tPA binding site on VSMC, an anti-p63 monoclonal antibody was found to block tPA binding. Furthermore, heterologous expression of an N-terminally truncated mutant of p63, which targets exclusively to the plasma membrane, led to an increase in tPA-catalyzed plasminogen activation. Therefore, p63 on the surface of VSMC may contribute to the functional regulation of the plasminogen activation system in the vessel wall.

Published
2003

18. Plasminogen Activators: Structure and Function

Author

Vincent Ellis

Subjects
Serine protease, Proteases, biology, Chemistry, Plasmin, Trypsin, Tissue plasminogen activator, Cell biology, Serine, biology.protein, medicine, Extracellular Matrix Degradation, Plasminogen activator, medicine.drug
Abstract

Mammalian species have two plasminogen activators, urokinase plasminogen activator (uPA) and tissue-type plasminogen activator (tPA), that are the products of separate genes and members of the trypsin family of serine proteases. Both are mosaic proteins with modular structures similar to the related blood coagulation proteases. The two plasminogen activators provide an excellent example of the regulatory potential made available by such modular construction. Although catalyzing the same reaction, that is, specific hydrolysis of Arg560–Val561 of plasminogen, gross differences in the organization of the N-terminal modules of the plasminogen activators, together with subtle differences in the serine protease domain, lead to remarkably different functional properties. These functional properties reflect the differing biological roles of the two plasminogen activators. The activity of tPA is strongly enhanced by fibrin, and tPA is therefore predominantly responsible for plasmin-catalyzed fibrin dissolution in the maintenance of vascular haemostasis. By contrast, the activity of uPA is regulated by interactions at the surface of cells. Therefore, uPA is thought to be primarily responsible for generating pericellular plasmin activity and contributes to the proteolytic activities involved in extracellular matrix degradation and other mechanisms that regulate cellular behavior. Although the two plasminogen activators have well-defined roles in these processes, recent observations have suggested that they also have some overlap of function as well as some previously unsuspected functions.

Published
2003

19. Plasminogen activation at the cell surface

Author

Vincent Ellis

Subjects
Proteases, Protease, Plasmin, medicine.medical_treatment, Integrin, Cell migration, Biology, Urokinase receptor, Biochemistry, medicine, biology.protein, Transcriptional regulation, Plasminogen activator, medicine.drug
Abstract

It has been emphasized here that plasminogen represents an enormous reservoir of proteolytic potential and that its activation is consequently a highly regulated process. This begins at the level of transcriptional regulation of the two plasmino-gen activators and in some cell types also their regulated secretion. However, the functional regulation of the plasminogen activators is the level at which the com-plexity of this proteolytic system is most apparent. It is now clear that a diversity of mechanisms exist to regulate the activation and activity of the plasminogen activa-tors, and that these include the utilization of these soluble proteins as cell-surface proteases. uPA is clearly the primary plasminogen activator in this context, binding uPAR and forming catalytic complexes that generate plasmin activity with very high efficiency, and furthermore cooperating with protease inhibitors to confine this ac-tivity to the cell surface or pericellular environment. The activity of this proteolytic system, which is thought to be involved in mediating invasive cellular migration, appears to be functionally linked to other systems fundamental to this cellular behavior. A variety of mechanisms have been proposed, but a common feature is direct or indirect interactions with integrins potentially leading to signaling to the cellular cytoskeletal machinery, suggesting a cooperativity between these systems in mediating invasive migration. tPA clearly also has the potential to act as a cell-surface protease, in addition to its fibrin-dependent role in vascular hemostasis. A variety of cellular binding sites for tPA have been identified, some of which appear to regulate plasminogen activation as efficiently as uPAR. In contrast to uPAR, these binding sites may be cell-type specific, although their roles in vivo have yet to be established.

Published
2003

20. Transcriptional and post-transcriptional regulation of the receptor for urokinase-type plasminogen activator by cytokines and tumour promoters in the human lung carcinoma cell line A549

Author

C Pyke, Keld Danø, Leif R. Lund, Vincent Ellis, and Ebbe Rønne

Subjects
Transcription, Genetic, Plasmin, medicine.medical_treatment, Basic fibroblast growth factor, Receptors, Cell Surface, Biology, Biochemistry, Receptors, Urokinase Plasminogen Activator, Enzyme activator, chemistry.chemical_compound, Epidermal growth factor, medicine, Tumor Cells, Cultured, Humans, RNA, Messenger, RNA Processing, Post-Transcriptional, skin and connective tissue diseases, Molecular Biology, Protein Kinase C, Urokinase, Epidermal Growth Factor, Growth factor, Cell Membrane, Cell Biology, Molecular biology, Urokinase-Type Plasminogen Activator, Cell biology, Urokinase receptor, Enzyme Activation, chemistry, Carcinogens, Cytokines, Tetradecanoylphorbol Acetate, Plasminogen activator, medicine.drug, Research Article
Abstract

The receptor for urokinase-type plasminogen activator (uPAR) is an integral membrane protein that specifically binds urokinase-type plasminogen activator (uPA) and plays a crucial role in cell surface plasmin generation. We have previously found that transforming growth factor-beta, type 1 (TGF-beta 1), increases uPAR gene transcription in the human lung carcinoma cell line A549 and now report that also epidermal growth factor (EGF) and the tumour promoter phorbol 12-myristate 13-acetate (PMA) cause increased uPAR transcription and that PMA and TGF-beta 1 in addition increase the stability of uPAR mRNA, while EGF has no effect on this parameter. All three compounds also increase the uPAR protein level, as measured by cell-binding experiments with radiolabelled ligand. The increase in uPAR protein level was however considerably lower with all three compounds than the increase in mRNA level, suggesting that they also exert a translational or post-translational control. Accompanying the increase in the number of uPAR molecules there was a proportional decrease in their ligand-binding affinity, the mechanism of which is unknown. Platelet-derived growth factor, basic fibroblast growth factor and cyclic AMP analogues did not induce any change in the uPAR mRNA level in A549 cells. Previous studies have shown that expression of uPA and its type-1 inhibitor is regulated by a variety of cytokines in a cell-specific manner. The present study indicates that cytokines in addition influence cell surface plasminogen activation by regulating uPAR expression.

Published
1995

21. Ligand interaction between urokinase-type plasminogen activator and its receptor probed with 8-anilino-1-naphthalenesulfonate. Evidence for a hydrophobic binding site exposed only on the intact receptor

Author

Keld Danø, Vincent Ellis, and Michael Ploug

Subjects
Receptors, Cell Surface, Ligands, Biochemistry, Anilino Naphthalenesulfonates, Receptors, Urokinase Plasminogen Activator, medicine, Chymotrypsin, Binding site, Receptor, Fluorescent Dyes, Urokinase, Binding Sites, biology, Chemistry, Hydrolysis, Antibodies, Monoclonal, Ligand (biochemistry), Urokinase-Type Plasminogen Activator, Urokinase receptor, Spectrometry, Fluorescence, biology.protein, Biophysics, Vitronectin, Plasminogen activator, medicine.drug
Abstract

The cellular receptor for urokinase-type plasminogen activator (uPAR) is a glycolipid-anchored membrane protein thought to play a primary role in the generation of pericellular proteolytic activity, and to be involved in cancer cell invasion and metastasis. This protein is composed of three homologous domains, the NH2-terminal of which is involved in the high-affinity binding (Kd approximately 0.1-1.0 nM) to the epidermal growth factor-like module of urokinase-type plasminogen activator (uPA). Here we report that intact uPAR binds the low molecular weight fluorophore 8-anilino-1-naphthalenesulfonate (ANS) to form a 1:1 stoichiometric complex and that the resulting enhancement of the ANS fluorescence probes the functional state of uPAR as judged by several independent criteria. First, the uPAR-mediated increase in ANS fluorescence can be titrated by uPA as well as by its receptor binding derivatives (the amino-terminal fragment and the growth factor-like module). Second, an anti-uPAR monoclonal antibody, capable of preventing uPA binding, can also titrate the uPAR-dependent ANS fluorescence whereas other antibodies not interfering with uPA binding are unable to exert this effect. Third, the dissociation profile of uPA-uPAR complexes as a function of increasing concentrations of guanidine hydrochloride closely parallels the loss of the ANS binding site in uPAR. Finally, liberation of the NH2-terminal domain from uPAR by limited chymotrypsin cleavage after Tyr87 leads to a loss of both enhanced ANS fluorescence and high-affinity uPA binding.(ABSTRACT TRUNCATED AT 250 WORDS)

Published
1994

22. Potentiation of plasminogen activation by an anti-urokinase monoclonal antibody due to ternary complex formation. A mechanistic model for receptor-mediated plasminogen activation

Author

Keld Danø and Vincent Ellis

Subjects
Plasmin, Protein Conformation, Molecular Sequence Data, Antigen-Antibody Complex, Biochemistry, Models, Biological, Kringle domain, Zymogen, medicine, Humans, Enzyme kinetics, Amino Acid Sequence, Fibrinolysin, Binding site, Protein Precursors, Molecular Biology, Ternary complex, Urokinase, Chemistry, Hydrolysis, Antibodies, Monoclonal, Plasminogen, Cell Biology, Urokinase-Type Plasminogen Activator, Kinetics, Immunoglobulin G, Biophysics, Immunoglobulin Heavy Chains, Plasminogen activator, medicine.drug
Abstract

We have observed that a murine IgG1 monoclonal antibody directed against human urokinase-type plasminogen activator (uPA) greatly potentiates pro-uPA-mediated plasminogen activation. This effect was dependent on the interaction between the immunoglobulin and the kringle domain of pro-uPA and could be competed efficiently by kringle-containing proteolytic fragments of uPA. In addition, the potentiation could also be competed by the lysine analog 6-aminohexanoic acid, an antagonist of plasminogen binding. This unexpected plasminogen binding dependence was found to be due to a carboxyl-terminal lysine residue on the immunoglobulin gamma chain, which by analogy with other proteins represents a potential binding site for plasminogen. Removal of this residue with carboxypeptidase B resulted in a complete abolition of the potentiation. It appears therefore that the potentiatory effect involves a novel mechanism with the antibody acting to provide a specific template for the assembly of a ternary complex involving pro-uPA/uPA and plasminogen, enabling them to interact in a catalytically favorable manner. This interpretation was confirmed by studying the kinetics of plasminogen activation by the complex between active, two-chain uPA and the antibody, which resulted in an overall 50-fold increase in reaction efficiency (kcat/Km), primarily due to a reduction in Km from 20 to 0.1 microM. Pro-uPA activation by plasmin was also accelerated, although to a lesser extent. The potentiation due to complex formation also provides a mechanism for the initiation of this system, dependent only on the low intrinsic proteolytic activity of the zymogen forms. The effects observed here, mediated by ternary complex formation, simulate the effects we have previously observed on assembly of the uPA receptor-mediated cellular plasminogen activation system and may therefore represent a mechanistic model for both its activity and initiation.

Published
1993

23. [14] Cellular receptor for urokinase-type plasminogen activator: Function in cell-surface proteolysis

Author

Niels Behrendt, Keld Danø, and Vincent Ellis

Subjects
Urokinase, Protease, medicine.diagnostic_test, Plasmin, Chemistry, medicine.medical_treatment, Proteolysis, Cell membrane, Urokinase receptor, medicine.anatomical_structure, Biochemistry, Cell surface receptor, medicine, Plasminogen activator, medicine.drug
Abstract

Publisher Summary This chapter discusses the methods that are developed for the study of urokinase-type plasminogen activator (uPa) and plasmin activity in relation to urokinase-type plasminogen activator (uPAR). These methods may also have a more general applicability in the study of other cell surface-associated protease systems, particularly, those that may have an intimate involvement with the plasminogen activation system, for example, the matrix metalloproteases. Numerous studies have delineated a system whereby the generation of cell surface proteolytic activity can be mediated by uPAR, the cellular receptor for the urokinase-type plasminogen activator (uPA). Because of the saturability of the inhibitory effect of isolated uPAR it is possible, under the experimental conditions to derive an approximation to the dissociation constant for the uPA-uPAR interaction in solution. The requirement for quantitative assays to investigate the functional effects of cell surface uPAR on the activity of the uPA-catalyzed plasminogen activation system presents a number of difficulties, particularly with respect to sensitivity and specific quantification.

Published
1993

24. A Key Molecule Dictating and Regulating Surface Plasmin Formation : The Receptor for Urokinase Plasminogen Activator

Author

Vincent Ellis, Niels Behrendt, Ettore Appella, M. Vittoria Cubellis, Keld Danø, Ann Louring Roldan, Francesco Blasi, and M T Masucci

Subjects
Extracellular matrix, Urokinase receptor, medicine.anatomical_structure, Plasmin, Chemistry, Cell, medicine, Proteolytic enzymes, Extracellular, Cell migration, Plasminogen activator, medicine.drug, Cell biology
Abstract

Regulation of cell to cell contacts and of cell migration is thought to require the action of protease systems which are needed to sever the ties that link cells to other cells and to the extracellular matrix, and to overcome barriers like the basement membranes. Since cell migration phenomena occur from gametogenesis through embryonic development to adulthood, and since also many pathological disorders are associated with or require tissue destruction and cell migration, the requirement for extracellular proteolytic enzymes is a very widespread phenomenon, which however has not yet been clearly understood on a molecular biological and biochemical basis.1–3

Published
1990

27. Inhibition of prothrombinase complex by plasma proteinase inhibitors

Author

Vijay V. Kakkar, Vincent Ellis, and Michael F. Scully

Subjects
Blood Platelets, Antithrombin III, Phospholipid, Phosphatidylserines, Biochemistry, chemistry.chemical_compound, Thrombin, Reaction rate constant, Prothrombinase, medicine, Animals, Humans, Platelet, Vesicle, Platelet Factor 3, Antithrombin, Factor V, Kinetics, chemistry, Factor Va, alpha 1-Antitrypsin, Factor X, Factor Xa, Liposomes, Phosphatidylcholines, Cattle, medicine.drug
Abstract

The rate of inactivation of human coagulation factor Xa by the plasma proteinase inhibitors antithrombin III and alpha 1-antitrypsin has been studied in the presence of the accessory components which constitute the prothrombinase complex. The rate of inactivation of factor Xa by antithrombin III was found to be decreased in the presence of phospholipid vesicles with high affinity for factor Xa. The second-order rate constant for the reaction fell from 6.21 X 10(4) to 3.40 X 10(4) M-1 min-1 in the presence of 20 microM phospholipid. Purified factor Va had no effect on the rate of inactivation of factor Xa in the absence of phospholipid. In the presence of phospholipid, factor Va increased the protective effect displayed by phospholipid, further reducing the rate constant to 2.20 X 10(4) M-1 min-1. The rate of inactivation of factor Xa by alpha 1-antitrypsin was unaffected under these conditions. Platelet-bound prothrombinase complex was formed by incubation of factor Xa with washed human platelets activated by a mixture of collagen and thrombin. The prothrombinase activity was inhibited by antithrombin III was a second-order rate constant of 0.85 X 10(4) M-1 min-1. This rate was obtained in both the presence and absence of exogenous factor Va. Platelet factor 3 vesicles, isolated from platelet aggregation supernatants, also formed prothrombinase complex in the presence of factor Va, and this was inhibited by antithrombin III at the same rate as the platelet-bound complex. There was no protection of the platelet-bound prothrombinase complex from inhibition by alpha 1-antitrypsin.

Published
1984

28. The receptor for urokinase-type plasminogen activator is deficient on peripheral blood leukocytes in patients with paroxysmal nocturnal hemoglobinuria

Author

Torben Plesner, Gunilla Høyer-Hansen, Vincent Ellis, Keld Danø, Ebbe Rønne, Michael Ploug, and Niels Ebbe Hansen

Subjects
Immunology, Hemoglobinuria, Paroxysmal, Receptors, Cell Surface, Biochemistry, Receptors, Urokinase Plasminogen Activator, Flow cytometry, Mice, Cell surface receptor, hemic and lymphatic diseases, Leukocytes, medicine, Animals, Humans, Receptor, Urokinase, biology, medicine.diagnostic_test, Fibrinolysis, Plasminogen, Cell Biology, Hematology, Flow Cytometry, medicine.disease, Urokinase-Type Plasminogen Activator, biology.protein, Paroxysmal nocturnal hemoglobinuria, Hemoglobinuria, Antibody, Plasminogen activator, medicine.drug
Abstract

Paroxysmal nocturnal hemoglobinuria (PNH) is an acquired clonal defect in bone marrow-derived cells and is clinically associated with intravascular hemolysis, hemoglobinuria, and an increased frequency of venous thrombosis. The common denominator of PNH-affected blood cells appears to be a defect in the membrane attachment of proteins normally anchored by glycosyl-phosphatidylinositol (GPI). We report here that the cellular receptor for urokinase-type plasminogen activator (u-PAR) is deficient on affected peripheral blood monocytes and granulocytes from four individuals with PNH as evidenced by chemical cross-linking analysis as well as by immunofluorescence flow cytometry using a monoclonal anti-u-PAR antibody. In contrast, on normal blood monocytes and granulocytes we find significant amounts of u-PAR, which is attached to the plasma membrane by a GPI-anchor as defined by its sensitivity towards a specific phospholipase treatment. By two-color flow cytometry it was shown that deficiency of u-PAR expression paralleled that of another GPI-anchored protein. As u-PAR is involved in the initiation of pericellular proteolysis, the reduced expression of u-PAR on PNH-affected leukocytes led to an overall reduction in the capacity for plasminogen activation by cell-surface-bound urokinase. Whereas the abnormal susceptibility of PNH-affected erythrocytes to lysis by autologous complement has been related to the low expression of three GPI-anchored complement regulatory proteins on the cell surface, we now propose that lack of u-PAR expression on the surface of peripheral blood leukocytes may be causally related to the high incidence of venous thrombosis observed in PNH patients.

29. Plasminogen activation by receptor-bound urokinase. A kinetic study with both cell-associated and isolated receptor

Author

Niels Behrendt, Keld Danø, and Vincent Ellis

Subjects
Plasmin, Biochemistry, Catalysis, Cell Line, chemistry.chemical_compound, Plasminogen Activators, Cell surface receptor, Antifibrinolytic agent, medicine, Humans, Fibrinolysin, Receptor, Molecular Biology, Urokinase, U937 cell, Plasminogen, Cell Biology, Urokinase-Type Plasminogen Activator, Antifibrinolytic Agents, Cell biology, Kinetics, chemistry, Phorbol, Electrophoresis, Polyacrylamide Gel, Plasminogen activator, medicine.drug
Abstract

The specific cellular receptor for urokinase-type plasminogen activator (uPA) is found on a variety of cell types and has been postulated to play a central role in the mediation of pericellular proteolytic activity. We have studied the kinetics of plasminogen (Plg) activation catalyzed by uPA specifically bound to its receptor on the human monocytoid cell-line U937 and demonstrate this process to have properties differing widely from those observed for uPA in solution. The solution-phase reaction was characterized by a Km of 25 microM and for the cell-associated reaction this fell 40-fold to 0.67 microM, below the physiological Plg concentration of 2 microM. A concomitant 6-fold reduction in kcat resulted in an increase in the overall catalytic efficiency, kcat/Km, of 5.7-fold. This high affinity Plg activation was abolished in the presence of a Plg-binding antagonist. In contrast to intact cells, purified uPA receptor (isolated from phorbol 12-myristate 13-acetate-stimulated U937 cells) was observed to partially inhibit uPA-catalyzed Plg activation, although activity against low molecular weight substrates was retained. Therefore, the cellular binding of Plg appears to be of critical importance for the efficient activation of Plg by receptor-bound uPA. Plasmin generated in the cell-surface Plg activation system described here was also observed to be protected from its principal physiological inhibitor alpha-2-antiplasmin. Together, these data demonstrate that the cell surface constitutes the preferential site for Plg activation when uPA is bound to its specific cellular receptor, which therefore has the necessary characteristics to play an efficient role in the generation of pericellular proteolytic activity.

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