Your search keyword '"Protein C Inhibitor"' showing total 50 results

1. Host protein C inhibitor inhibits tumor growth, but promotes tumor metastasis, which is closely correlated with hypercoagulability.

Author

Nobuyuki Akita, Ning Ma, Takayuki Okamoto, Kunihiro Asanuma, Kakunoshin Yoshida, Junji Nishioka, Motomu Shimaoka, Koji Suzuki, and Tatsuya Hayashi

Subjects

*PROTEIN C inhibitor, *TUMOR growth, *METASTASIS, *HYPERCOAGULATION disorders, *IMMUNOHISTOCHEMISTRY, *LABORATORY mice

Abstract

Introduction: Protein C inhibitor (PCI), a member of the serine protease inhibitor family, is expressed in various human tissues, including liver and kidneys. In the plasma, PCI physiologically inhibits an anticoagulant serine protease, activated protein C (APC). PCI expressed by cancer cells suppresses tumor invasion by inhibiting urokinase-type plasminogen activator, and inhibits tumor growth and metastasis, which are independent of its protease-inhibitory activity. In the present study, we clarified the effects of host PCI on growth and metastasis of B16 melanoma (B16) cells by comparing between wild-type mice and mice transgenic for human PCI gene (hPCI-TG), which have a tissue distribution of PCI similar to that observed in humans. Materials and Methods: Growth of intracutaneously-injected B16 cells was evaluated by measuring the tumor volume, and metastatic behavior of intravenously-injected B16 cells by counting the number of metastatic lung nodules. Results: Growth of intracutaneously injected B16 cells was significantly faster in wild-type mice than in hPCI-TG mice; however, hPCI-TG mice developed more metastatic nodules of B16 cells in the lungs. Immunohistochemical analysis using anti-mouse fibrinogen antibody revealed more fibrin deposition in the lung in hPCI-TG mice than in wild-type mice. Furthermore, the more invasive behavior observed in hPCI-TG mice was reduced by rabbit anti-human PCI IgG, APC, or soluble TM administration for 3 consecutive days including the day that B16 cells were injected. Conclusion: Our results suggest that like PCI expressed in tumor cells, host PCI also inhibits tumor growth, but host PCI promotes tumor metastasis via its procoagulant properties. [ABSTRACT FROM AUTHOR]

Published

2015

2. Diversity of Human Plasma Protein C Inhibitor

Author

Saito, Akio

Subjects

*BLOOD plasma, *PROTEIN C inhibitor, *DERMATAN sulfate, *HYDROXYAPATITE, *ION exchange (Chemistry), *MATRIX-assisted laser desorption-ionization, *TIME-of-flight mass spectrometry, *PHOSPHORYLATION

Abstract

Abstract: Protein C inhibitor was purified from human plasma by use of a dermatan sulfate or heparin column, followed by hydroxyapatite, gel filtration and ion exchange columns. A dimer of protein C inhibitor was detected by SDS-PAGE under reducing conditions, in addition to two forms of monomer species. One of the monomers, 52-kDa PCI, formed a stable complex with activated protein C, urokinase, plasma and tissue kallikrein, but the dimer species and 48-kDa PCI were inactive. When the monomer and dimer forms of protein C inhibitor were applied to 2D-PAGE, more than 20 spots were observed by Western blot analysis and were confirmed to be protein C inhibitor by MALDI-TOF mass spectrometry. The heterogeneity of the protein C inhibitor species was not due to glycosylation or phosphorylation. [Copyright &y& Elsevier]

Published

2012

3. The APC-PCI concentration as an early marker of activation of blood coagulation: A study of women on combined oral contraceptives

Author

Bremme, K., Hamad, R. Rafik, Berg, Elisabeth, Strandberg, K., and Stenflo, J.

Subjects

*VENOUS thrombosis risk factors, *BLOOD coagulation, *ORAL contraceptives, *PROTEIN C inhibitor, *MENSTRUAL cycle, *DISEASES in women, *BLOOD plasma

Abstract

Abstract: Background: The risk of venous tromboembolism (VTE) in women taking combined oral contraceptives (COCs) is attributed to changes in coagulation and fibrinolysis. The impact of the COCs may be greater in women with preexisting thrombophilic defects. Nevertheless most women who suffer from venous thrombosis do not have any of the well known hereditary or acquired risk factors. A simple and sensitive marker of”thrombogenicity” has not been identified. Objectives: To investigate the effects of two different monophasic combined oral contraceptives (COCs) on the plasma concentrations of activated protein C-inhibitor of protein C ( APC-PCI) and on comparable hemostatic factors in fertile women. Method: Forty four healthy nulliparous women with regular menstrual periods were included and randomly assigned to start with a monophasic preparation containing 30μg ethinylestradiol and 150μg levonogestrel (LNG/EE) or a preparation containing 30μg ethinylestradiol and 150 ug desogestrel (DG/EE). After a wash out period of two months, treatment with the alternate preparation was initiated and continued for two more cycles. Results: The plasma concentration of the APC-PCI complex and thrombin-antithrombin complex (TAT) increased during treatment with the two COCs. During DG/EE treatment the APC-PCI complex increased significantly more than during LNG/EE (p<0,01).The plasma concentration of D-dimer did not increase during OC treatment. Conclusion: The APC-PCI complex concentration, which serves as a marker for thrombin generation and indicates hypercoagulability, was increased during COC treatment compared to baseline. The method is a sufficiently sensitive marker to detect even small differences in the activation of coagulation. [Copyright &y& Elsevier]

Published

2012

4. Determination of alpha-2-macroglobulin complexes by a new immuno-activity assay

Author

Atkinson, Helen M., Parmar, Nagina, Berry, Leslie R., and Chan, Anthony K.C.

Subjects

*THROMBIN, *PROTEIN C inhibitor, *ANTITHROMBINS, *HEPARIN, *PROTEASE inhibitors, *HEMOSTATICS, *PROTHROMBIN

Abstract

Abstract: Introduction: Alpha-2-macroglobulin (α2M) is a broad specificity protease inhibitor which impacts several hemostatic pathways. Selective detection of various α2M complexes may be useful to define markers for the status of different hemostatic components. We present proof of principle for a novel assay to quantitatively measure α2M in complex with a variety of hemostatic factors. Materials and Methods: The assay makes use of the fact that α2M entraps proteases within a molecular “cage”, leaving them inaccessible to macromolecular substrates while retaining functionality against small synthetic substrates. Wells coated with anti-α2M antibodies were used to isolate the complexes from buffer or plasma, followed by detection of specific proteases with chromogenic substrates. Macromolecular inhibitors were added to eliminate signal from any unbound proteases. Results: Calibration curves constructed with purified protease-α2M complexes were sigmoidal in nature, as is typical with immuno-assays. The specificity of signal production was confirmed with inhibitors that target either free protease, or both free and α2M-bound protease. The detection range of the assay was dependent on the protease being measured, and the surrounding matrix. Interference in detection of complexes in plasma was found to be caused, in part, by free α2M. Thrombin-α2M complexes were quantified in adult and newborn plasma following induction of thrombin generation and found to be significantly higher in adults, likely due to higher prothrombin levels. Conclusions: This assay provides a versatile platform method for quantification of multiple protease-α2M complexes. It may prove useful for mechanistic in vitro studies of hemostatic pathways, and potentially for clinical applications. [Copyright &y& Elsevier]

Published

2012

5. Early identification of acute myocardial infarction by activated protein C–protein C inhibitor complex

Author

Bhiladvala, Pallonji, Strandberg, Karin, Stenflo, Johan, and Holm, Johan

Subjects

*PROTEIN C, *CREATINE kinase, *MYOCARDIAL infarction, *GLYCOPROTEINS

Abstract

Abstract: Introduction: Increased coagulation activity due to coronary thrombosis in a ruptured plaque should result in activation of the protein C anticoagulant system with formation of complexes between activated protein C (APC) and the protein C inhibitor (PCI), which reflects coagulation activity. We hypothesized that elevated APC-PCI concentration might allow earlier detection of ongoing myocardial infarction than traditional biochemical markers. We have evaluated a newly devised immunofluorimetric assay for measuring plasma concentration of APC-PCI complexes among patients with suspected acute coronary syndrome. Materials and methods: Blood samples were taken from 340 patients (median 71 years, range 31–97) with suspected acute coronary syndrome at first presentation in the emergency department. Electrocardiogram was recorded and APC-PCI, Troponin I and Creatine kinase-MB concentrations were repeatedly measured 3 times at 6 h interval. Results: The 74 patients who were eventually diagnosed with myocardial infarction had a higher median level of APC-PCI complex than those without myocardial damage; 0.27 vs. 0.20 μg/L (p =0.001). In a multivariate regression model, APC-PCI level in the fourth quartile (>0.32 μg/L) independently predicted myocardial infarction with an odds ratio of 3.7 (95% CI 1.4–9.6, p <0.01). Conclusion: Early APC-PCI elevation can be detected among patients with a normal first Troponin I and non-ST-elevation myocardial infarction and provides additional risk assessment in acute coronary syndrome. [Copyright &y& Elsevier]

Published

2006

6. Role of each Asn-linked glycan in the anticoagulant activity of human protein C inhibitor

Author

Fujita, Mitsugu, Izutani, Wakako, Takahashi, Kenichi, Nishizawa, Koji, Shirono, Hiroyuki, and Koga, Junichi

Subjects

*PROTEIN C, *ASPARAGINE, *ANTICOAGULANTS

Abstract

The N-glycosylation site mutants of human protein C inhibitor (PCI; N230S, N243Q, N319Q, N230S/N243Q, and N230S/N319Q) were prepared by amino acid replacement of the asparagine residue with a serine or glutamine residue using site-directed mutagenesis and expressed in the baculovirus/insect cell expression system. To examine the importance of each Asn-linked glycan in the activity of PCI, we compared wtPCI with the mutants of N-glycosylation site(s) in terms of the procoagulant protease-inhibitory and anticoagulant activities. The inhibitory activities of N230S, N319Q, and N230S/N319Q toward human thrombin and plasma kallikrein were significantly increased compared with wtPCI, but those of N243Q and N230S/N243Q were reduced. The inhibitory activity of N230S toward human plasma coagulation was significantly increased compared with wtPCI, and that of N230S/N319Q was also significantly increased compared with N319Q. Furthermore, the procoagulant protease-inhibitory and anticoagulant activities of N230S/N319Q (glycosylated on Asn243 only) compared favorably with those of N230S, and both of the mutants possessed highest activities in the purified mutants. These results suggest that the Asn243-linked glycan in PCI molecule possesses critical roles for its anticoagulant activity in the circulation, and the Asn230-linked glycan down-regulates the activity of PCI. [Copyright &y& Elsevier]

Published

2002

7. Identification of novel small molecule inhibitors of activated protein C

Author

Gerry A. F. Nicolaes, Olivier Sperandio, Roy Schrijver, Bruno O. Villoutreix, Karin C. A. A. Wildhagen, Simone J.H. Wielders, Promovendi CD, Ondersteunend personeel CD, Biochemie, and RS: CARIM - R1 - Thrombosis and haemostasis

Subjects

Models, Molecular, Virtual screening, Protein Data Bank (RCSB PDB), Drug Evaluation, Preclinical, Drug design, Small Molecule Libraries, Structure-Activity Relationship, Thrombin, medicine, Humans, Binding site, Protein C Inhibitor, chemistry.chemical_classification, Binding Sites, Chemistry, Binding protein, Hematology, computer.file_format, Surface Plasmon Resonance, Protein Data Bank, Small molecule, Enzyme, Activated protein C, Biochemistry, Factor Va, computer, medicine.drug, Protein C

Abstract

Introduction Activated protein C (APC) is the central enzyme of the anticoagulant protein C pathway. Low concentrations of APC circulate in plasma and are believed to contribute to the maintenance of a normal haemostatic balance. Materials and Methods We have used a structure-based virtual screening approach to discover small drug-like molecules that inhibit the interaction between APC and its substrate FVa through inhibition of a predominant APC exosite, known to be involved in FVa substrate binding. We have combined in silico selection with functional screening and direct binding analysis to identify novel molecules and to ascertain and characterize the inhibition of the interaction between APC and FVa. Results We have identified a number of novel molecules that bind to APC and protein C with Kd values in the range of 10 -3 – 10 -5 M. Inhibition by these molecules is incomplete, which most likely reflects the extended surface that is involved in the interaction between APC and its substrates. Direct binding of hit molecules to variant APC molecules that were mutated in the targeted binding site revealed that several of the molecules presented a 100–500 fold lower affinity for the variant molecule, suggesting that these molecules indeed bind the exosite of APC. Conclusions The protein-protein interaction inhibitors discovered here, could function as starting molecules for further development of small molecules with anti-APC properties. Such molecules may be of clinical interest, in particular in individuals where thrombin formation is compromised and the haemostatic balance is tipped towards bleeding tendencies, such as in haemophilia A.

Published

2014

8. Diversity of Human Plasma Protein C Inhibitor

Author

Akio Saito

Subjects

Glycosylation, Dimer, Protein C inhibitor, Molecular Sequence Data, Dermatan Sulfate, Dermatan sulfate, chemistry.chemical_compound, Western blot, medicine, Humans, Amino Acid Sequence, Plasma Kallikrein, Protein C Inhibitor, Kunitz STI protease inhibitor, medicine.diagnostic_test, Hematology, Urokinase-Type Plasminogen Activator, Monomer, chemistry, Biochemistry, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, Phosphorylation, Electrophoresis, Polyacrylamide Gel, Protein Multimerization, Tissue Kallikreins, Protein C

Abstract

Protein C inhibitor was purified from human plasma by use of a dermatan sulfate or heparin column, followed by hydroxyapatite, gel filtration and ion exchange columns. A dimer of protein C inhibitor was detected by SDS-PAGE under reducing conditions, in addition to two forms of monomer species. One of the monomers, 52-kDa PCI, formed a stable complex with activated protein C, urokinase, plasma and tissue kallikrein, but the dimer species and 48-kDa PCI were inactive. When the monomer and dimer forms of protein C inhibitor were applied to 2D-PAGE, more than 20 spots were observed by Western blot analysis and were confirmed to be protein C inhibitor by MALDI-TOF mass spectrometry. The heterogeneity of the protein C inhibitor species was not due to glycosylation or phosphorylation.

Published

2012

9. Haplotypes of the endothelial protein C receptor gene and Behçet's disease

Author

Jordi Fontcuberta, Francisco España, Laura Martos, Amparo Vayá, Amparo Estellés, José M. Ricart, Silvia Navarro, Pilar Medina, José Todolí, and Elena Bonet

Subjects

Adult, Male, Adolescent, Protein C inhibitor, Receptors, Cell Surface, Comorbidity, Behcet's disease, Young Adult, Von Willebrand factor, Antigens, CD, Risk Factors, Prevalence, medicine, Humans, Genetic Predisposition to Disease, Child, Aged, Endothelial protein C receptor, biology, business.industry, Behcet Syndrome, Haplotype, C-reactive protein, Endothelial Protein C Receptor, Thrombosis, Hematology, Middle Aged, medicine.disease, Venous thrombosis, Haplotypes, Spain, Child, Preschool, Immunology, biology.protein, Female, business, Protein C, medicine.drug

Abstract

Introduction Behcet's disease is a vasculitis of unknown cause in which thrombosis occurs in about 25% of patients. Two haplotypes of the endothelial protein C receptor gene, H1 and H3, are associated with the risk of thrombosis. Thus, the objective of this study was to evaluate the influence of these haplotypes on the thrombosis risk in Behcet's disease. Material and Methods We evaluated the H1 and H3 haplotypes in 87 patients with Behcet's disease, 19 with and 68 without a history of thrombosis, and in 260 healthy individuals. We also measured protein C, activated protein C, and soluble endothelial protein C receptor levels in all individuals. Results The presence of the H1 haplotype seemed to protect Behcet's patients against thrombosis (odds ratio 0.21; 95% CI 0.1-0.8; p = 0.023), whereas the frequency of the H3 haplotype was lower in patients than in control individuals (0.19; 0.1-0.5; p = 0.006). Furthermore, the H1 haplotype was associated with increased levels of activated protein C, whereas the H3 haplotype was associated with the highest soluble endothelial protein C levels. Moreover, activated protein C levels were lower in patients with than in patients without posterior uveitis ( p Conclusions These findings indicate that the H1 haplotype protects Behcet's patients from thrombosis, likely via increased levels of activated protein C, whereas individuals carrying the H3 haplotype seem to be protected from the clinical manifestations associated with Behcet's disease, probably via increased soluble endothelial protein C levels.

Published

2012

10. Coagulation activation and ultrasound characteristics in patients with carotid artery disease

Author

Anders Gottsäter, Isabel Gonçalves, Tilo Kölbel, Stefan Acosta, Karin Strandberg, and Nuno Dias

Subjects

Male, medicine.medical_specialty, Amaurosis Fugax, Asymptomatic, Coronary artery disease, Carotid artery disease, medicine.artery, Internal medicine, medicine, Humans, Carotid Stenosis, cardiovascular diseases, Blood Coagulation, Stroke, Aged, Protein C Inhibitor, Ultrasonography, Aged, 80 and over, business.industry, Thrombin, Hematology, Amaurosis fugax, Middle Aged, Atherosclerosis, medicine.disease, Surgery, Stenosis, Ischemic Attack, Transient, Case-Control Studies, Cardiology, Female, medicine.symptom, Internal carotid artery, business, Protein C, Blood sampling

Abstract

INTRODUCTION: Elevated levels of markers for thrombin activation are associated with plaque echogenicity and degree of stenosis in patients with carotid artery stenosis. The Activated Protein C-Protein C Inhibitor (APC-PCI) complex reflects activation of the Protein C system and is a measure of thrombin generation. The aim of the present study was to examine APC-PCI complex in patients undergoing thrombendartherectomy for carotid artery stenosis, and to relate the findings to clinical characteristics and plaque morphology as determined by ultrasound. MATERIALS AND METHODS: Blood was obtained from 125 patients (39 female, median age 71 years) with carotid artery stenosis admitted from September 2005 to May 2007. The APC-PCI complex was measured using a sandwich immunofluorometric method and compared to an age- and sex-matched healthy control-group. Clinical and demographic characteristics, routine laboratory markers and ultrasound characteristics were analysed using univariate and multivariate analysis. RESULTS: APC-PCI complex concentration was significantly increased in patients with carotid artery stenosis (median 0.21 microg/L; 10th to 90th percentile 0.15-0.36) compared to a healthy control-group (0.19 microg/L; 0.11-0.31; P=.009). There was no significant difference in APC-PCI-values between asymptomatic (n=48) and symptomatic (n=77) patients with carotid artery stenosis (0.22 vs. 0.20 microg/L; p=0.626). Patients with minor stroke (n=31) had a higher median APC-PCI-concentration (0.27 microg/L; 0.15-0.63) than patients with amaurosis fugax (0.19 microg/L; 0.15-0.36) or transient ischemic attack (0.21 microg/L; 0.12-0.36) (p=0.016). No association was found between APC-PCI-values and the degrees of carotid artery stenosis or the time from the latest neurological symptoms to blood sampling. Patients with echolucent plaques had significantly lower APC-PCI concentrations (0.20 microg/L; 0.14-0.35 vs. 0.24 microg/L; 0.15-0.60; p=0.043), according to the Gray-Weale classification. CONCLUSIONS: Patients with carotid artery disease exhibit increased concentrations of APC-PCI compared to a healthy control-group, particularly those patients with echogenic plaques, who have significantly higher APC-PCI levels than patients with echolucent plaques. (Less)

Published

2010

11. Treatment of endothelium with the chemotherapy agent vincristine affects activated protein C generation to a greater degree in newborn plasma than in adult plasma

Author

Leslie R. Berry, Anthony K.C. Chan, Tracy Anne Mewhort-Buist, Sanjay Patel, Patricia C. Liaw, and Helen M. Atkinson

Subjects

Adult, Umbilical Veins, medicine.medical_specialty, Vincristine, Endothelium, Thrombomodulin, Protein C inhibitor, Flow cytometry, Plasma, Internal medicine, Humans, Medicine, Thromboplastin, alpha-Macroglobulins, Cells, Cultured, Protein C Inhibitor, medicine.diagnostic_test, business.industry, Age Factors, Infant, Newborn, Endothelial Cells, Membrane Proteins, Thrombosis, Blood Proteins, Hematology, Heparin, Antineoplastic Agents, Phytogenic, Endocrinology, medicine.anatomical_structure, alpha 1-Antitrypsin, business, Protein C, Protein Binding, medicine.drug

Abstract

Introduction Activated protein C (APC) is well-established as a physiologically important anticoagulant. During development, plasma concentrations of protein C and α 2 macroglobulin, factors involved in APC generation, differ from adult levels. Chemotherapy drugs can perturb endothelial expression of PC-activating receptors. This study examines the effect of chemotherapy treatment of endothelium on APC generation in newborn and adult plasma. Materials and methods APC generations were initiated on endothelial cells treated with vincristine or media by recalcifying defibrinated plasma with buffer containing thromboplastin. APC generation was terminated by mixing timed subsamples into FFRCMK-EDTA or heparin, followed by EDTA. APC-PCI and APC-α 1 AT were assayed by ELISA. APC-α 2 M was measured chromogenically. Since heparin converts free APC to APC-PCI, the difference between APC-PCI detected in heparin subsamples and APC-PCI detected in FFRCMK-EDTA subsamples gave the free APC. Cellular expression of EPCR and TM were measured by flow cytometry and Western blot. Results Vincristine-treated endothelium decreased free APC generation in newborn plasma to a greater degree than in adult plasma. APC-PCI levels in both adult and newborn plasma were unaffected by chemotherapy. Vincristine treatment reduced levels of APC-α 1 AT and APC-α 2 M to a greater degree in newborn plasma versus adult plasma. Expression of EPCR was reduced in cells treated with vincristine. Conversely, TM was reduced on the cell surface, but increased in whole cell lysates. Conclusions The differential response of newborn and adult plasma PC components to chemotherapy-mediated changes in cell surface components may be a factor in the increased risk of thrombosis in children receiving chemotherapy.

Published

2008

12. Redirection of the reaction between activated protein C and a serpin to the substrate pathway

Author

Peter A. Andreasen, Yu-ichi Kamikubo, Andras Gruber, Andrey A. Komissarov, Paul Declerck, and Aiwu Zhou

Subjects

Protein C inhibitor, Plasma protein binding, Serpin, Ligands, Protein Structure, Secondary, Epitope, law.invention, chemistry.chemical_compound, law, Sepsis, Plasminogen Activator Inhibitor 1, medicine, Humans, biology, Antibodies, Monoclonal, Hematology, Disseminated Intravascular Coagulation, Molecular biology, Recombinant Proteins, Spectrometry, Fluorescence, chemistry, Plasminogen activator inhibitor-1, biology.protein, Recombinant DNA, Electrophoresis, Polyacrylamide Gel, Vitronectin, Protein C, Protein Binding, medicine.drug

Abstract

Background Activated protein C (APC) reduces mortality in severe sepsis. Protecting APC in the circulatory system from inactivation by serine protease inhibitors (serpins) could improve its therapeutic efficiency. Significantly elevated levels of a serpin plasminogen activator inhibitor 1 (PAI-1) correlate with a lethal outcome in severe sepsis and disseminated intravascular coagulation. Intermolecular mechanisms were employed to redirect the reaction between APC and PAI-1 from the inhibitory to the substrate pathway, which results in the catalytic neutralization of the serpin. Methods The effects of anti-PAI-1 monoclonal antibodies (mAbs) and vitronectin, as well as their fragments, on the kinetics and stoichiometry of the reaction between PAI-1 and APC were studied using SDS PAGE and fluorescence spectroscopy. Results MAbs with epitopes at α-helix F redirected 70–80% of the reaction between PAI-1 and APC, to the substrate pathway. Vitronectin and its SMB domain did not affect the stoichiometry of acyl-enzyme formation, but enhanced the effect of mAbs. While vitronectin induced a more than two-fold increase in the rate of the reaction between PAI-1 and APC, neither mAbs (mAb fragments), nor SMB domain of vitronectin affected it. Conclusions Ligands interacting with α-helix F of PAI-1 demonstrated a potential for the protection of APC from inactivation by PAI-1. Since the mechanism of proteinase/serpin interaction is universal, a similar design and approach could be employed for enhancing the inactivation of other serpins in order to preserve APC activity in the circulation. Rational pharmacological targeting of the inhibitors of APC could have therapeutic utility.

Published

2008

13. The APC–PCI complex concentration predicts outcome of aortic surgery

Author

Karin Strandberg, Einar Vernersson, Gunnar Nilsson, Erik Berntorp, Johan Stenflo, and Jan Astermark

Subjects

Male, Critical Care, law.invention, Aortic aneurysm, law, Intensive care, medicine, Humans, Prospective Studies, cardiovascular diseases, Aged, Protein C Inhibitor, Aged, 80 and over, APACHE II, business.industry, Antithrombin, Hematology, Length of Stay, Middle Aged, medicine.disease, Intensive care unit, Abdominal aortic aneurysm, Treatment Outcome, Multiprotein Complexes, Anesthesia, Conventional PCI, Female, Complication, business, Aortic Aneurysm, Abdominal, Protein C, medicine.drug

Abstract

Introduction Coagulation activation may be related to complications during surgery for abdominal aortic aneurysm. The complex formed between activated protein C (APC) and the serpin, protein C inhibitor (PCI), is a sensitive indicator of the activation of blood coagulation. The purpose of the study was to establish whether the APC–PCI complex can provide information useful for the assessment of outcome after aortic surgery. Materials and methods In 38 patients, the APC–PCI complex was initially determined every 6 h and daily from day three. Protein C, antithrombin, global haemostatic tests, and clinical scores were investigated. Length of stay at the intensive care unit (ICU) and hospital, and vital status up to two years were recorded. Results The median APC–PCI complex concentration in samples drawn 0–6 h after surgery was more than 20-fold higher than the upper limit of the reference interval. The level then declined rapidly, but remained elevated during the first two days. In patients with higher initial APC–PCI complex concentrations, Sequential Organ Failure Assessment (SOFA) scores were higher, the ICU stay was longer, and survival up to two years was lower. Patients who did not survive the ICU care had higher APC–PCI complex levels at 6–12 h and 12–18 h. Conclusions High concentrations of the APC–PCI complex within 6–18 h after the aortic surgery predict a sinister outcome. The results suggest that the APC–PCI complex is indicative of the severity of the disease.

Published

2007

14. Alpha 2-macroglobulin enhances prothrombin activation and thrombin potential by inhibiting the anticoagulant protein C/protein S system in cord and adult plasma

Author

Martin Koestenberger, Gerhard Cvirn, Siegfried Gallistl, Bettina Leschnik, Wolfgang Muntean, and Joerg Kutschera

Subjects

Adult, Protein C inhibitor, Protein S, alpha-2-Macroglobulin, Thrombin, medicine, Humans, alpha-Macroglobulins, Dose-Response Relationship, Drug, biology, Chemistry, PROTHROMBIN FRAGMENT 1.2, Antithrombin, Infant, Newborn, Hematology, Fetal Blood, Molecular biology, Kinetics, Biochemistry, Mechanism of action, biology.protein, Electrophoresis, Polyacrylamide Gel, Prothrombin, medicine.symptom, Protein C, medicine.drug

Abstract

Protein S (PS) is a vitamin K-dependent plasma protein and serves as a cofactor for the anticoagulant activities of activated protein C (APC). We investigated the effects of different PS concentrations on prothrombin activation and thrombin generation in cord and adult plasma containing APC and different amounts of alpha 2-macroglobulin (a2-M). Prothrombin activation was assessed by monitoring the time-course of prothrombin fragment 1+2 (F1+2) generation. Thrombin generation curves were determined by means of a subsampling technique using the chromogenic substrate S-2238. We demonstrate a dose-dependent inhibition of the anticoagulant action of PS by a2-M: suppression of F1+2 and thrombin generation due to addition of PS was stronger in plasma containing low amounts of a2-M than in plasma with elevated a2-M levels. Since no complex formation between a2-M and PS was observed by means of SDS-PAGE, we attribute decreased anticoagulant action of PS at high a2-M levels to enhanced complex formation between APC and a2-M. Thereby, APC is subtracted from its cofactor PS, resulting in suppressed formation of the anticoagulant APC/PS complex. Thus, our data suggest that a2-M, besides its well-known anticoagulant effects, also acts as a procoagulant by suppressing the formation of the anticoagulant APC/PS complex. Our findings have implications particularly on thrombin generation and inhibition in cord plasma, since a2-M levels in newborns are elevated over adult values and the antithrombotic APC/PS pathway is up-regulated at birth. Therefore, elevated levels of a2-M might restrict the up-regulation of the APC/PS pathway.

Published

2002

15. Host protein C inhibitor inhibits tumor growth, but promotes tumor metastasis, which is closely correlated with hypercoagulability

Author

Nobuyuki Akita, Takayuki Okamoto, Tatsuya Hayashi, Kunihiro Asanuma, Junji Nishioka, Motomu Shimaoka, Koji Suzuki, Kakunoshin Yoshida, and Ning Ma

Subjects

Male, Pathology, medicine.medical_specialty, Lung Neoplasms, Time Factors, Protein C inhibitor, Thrombomodulin, Melanoma, Experimental, Mice, Transgenic, Biology, Metastasis, Immunoenzyme Techniques, Mice, medicine, Animals, Humans, Thrombophilia, Neoplasm Metastasis, Protein C Inhibitor, Coagulants, Hematology, medicine.disease, Immunohistochemistry, Mice, Inbred C57BL, Cancer cell, Conventional PCI, Cancer research, RNA, Female, therapeutics, Plasminogen activator, Protein C, Neoplasm Transplantation, medicine.drug

Abstract

Introduction Protein C inhibitor (PCI), a member of the serine protease inhibitor family, is expressed in various human tissues, including liver and kidneys. In the plasma, PCI physiologically inhibits an anticoagulant serine protease, activated protein C (APC). PCI expressed by cancer cells suppresses tumor invasion by inhibiting urokinase-type plasminogen activator, and inhibits tumor growth and metastasis, which are independent of its protease-inhibitory activity. In the present study, we clarified the effects of host PCI on growth and metastasis of B16 melanoma (B16) cells by comparing between wild-type mice and mice transgenic for human PCI gene (hPCI-TG), which have a tissue distribution of PCI similar to that observed in humans. Materials and Methods Growth of intracutaneously-injected B16 cells was evaluated by measuring the tumor volume, and metastatic behavior of intravenously-injected B16 cells by counting the number of metastatic lung nodules. Results Growth of intracutaneously injected B16 cells was significantly faster in wild-type mice than in hPCI-TG mice; however, hPCI-TG mice developed more metastatic nodules of B16 cells in the lungs. Immunohistochemical analysis using anti-mouse fibrinogen antibody revealed more fibrin deposition in the lung in hPCI-TG mice than in wild-type mice. Furthermore, the more invasive behavior observed in hPCI-TG mice was reduced by rabbit anti-human PCI IgG, APC, or soluble TM administration for 3 consecutive days including the day that B16 cells were injected. Conclusions Our results suggest that like PCI expressed in tumor cells, host PCI also inhibits tumor growth, but host PCI promotes tumor metastasis via its procoagulant properties.

Published

2014

16. Determination of alpha-2-macroglobulin complexes by a new immuno-activity assay

Author

Anthony K.C. Chan, Helen M. Atkinson, Leslie R. Berry, and Nagina Parmar

Subjects

Adult, Immunoassay, Proteases, Protease, biology, Chemistry, medicine.medical_treatment, Protein C inhibitor, Infant, Newborn, Reproducibility of Results, Hematology, Protease inhibitor (biology), In vitro, alpha-2-Macroglobulin, Thrombin, Biochemistry, Alpha 2-antiplasmin, medicine, biology.protein, Humans, alpha-Macroglobulins, medicine.drug, Peptide Hydrolases

Abstract

Introduction Alpha-2-macroglobulin (α 2 M) is a broad specificity protease inhibitor which impacts several hemostatic pathways. Selective detection of various α 2 M complexes may be useful to define markers for the status of different hemostatic components. We present proof of principle for a novel assay to quantitatively measure α 2 M in complex with a variety of hemostatic factors. Materials and Methods The assay makes use of the fact that α 2 M entraps proteases within a molecular “cage”, leaving them inaccessible to macromolecular substrates while retaining functionality against small synthetic substrates. Wells coated with anti-α 2 M antibodies were used to isolate the complexes from buffer or plasma, followed by detection of specific proteases with chromogenic substrates. Macromolecular inhibitors were added to eliminate signal from any unbound proteases. Results Calibration curves constructed with purified protease-α 2 M complexes were sigmoidal in nature, as is typical with immuno-assays. The specificity of signal production was confirmed with inhibitors that target either free protease, or both free and α 2 M-bound protease. The detection range of the assay was dependent on the protease being measured, and the surrounding matrix. Interference in detection of complexes in plasma was found to be caused, in part, by free α 2 M. Thrombin-α 2 M complexes were quantified in adult and newborn plasma following induction of thrombin generation and found to be significantly higher in adults, likely due to higher prothrombin levels. Conclusions This assay provides a versatile platform method for quantification of multiple protease-α 2 M complexes. It may prove useful for mechanistic in vitro studies of hemostatic pathways, and potentially for clinical applications.

Published

2011

17. Evaluation of two functional assays for protein C inhibitor/plasminogen activator inhibitor-3 activity

Author

Sylvia Hendl, Francisco España, Justo Aznar, Juan Gilabert, and Amparo Estellés

Subjects

Male, Genital Neoplasms, Female, Protein C inhibitor, Molecular Sequence Data, Enzyme-Linked Immunosorbent Assay, Sensitivity and Specificity, Andrology, Risk Factors, Thromboembolism, Blood plasma, medicine, Humans, Amino Acid Sequence, cardiovascular diseases, Incubation, Protein C Inhibitor, chemistry.chemical_classification, Heparin, Chemistry, Hematology, Pyrrolidonecarboxylic Acid, Plasminogen Inactivators, surgical procedures, operative, Enzyme, Chromogenic Compounds, Biochemistry, alpha 1-Antitrypsin, Conventional PCI, Female, Oligopeptides, Plasminogen activator, Protein C, medicine.drug

Abstract

Two functional assays for protein C inhibitor (PCI) were evaluated in parallel for the same plasma samples. One assay is specific for active PCI and measures its ability to form complexes with activated protein C (APC) in the presence of heparin (Espana et al, Thromb Res 64, 309, 1991) (Method A). After incubation of samples with heparin and an excess of APC, the amount of APC:PCI formed is measured by an ELISA. The second functional PCI assay is based on the determination of the residual amidolytic activity of the APC added to the sample. In all cases a good correlation was obtained with both methods. For 20 healthy subjects and 20 patients before surgery, there were no significant between-assay differences in the levels of functional PCI activity. On the other hand, there were significant between-assays differences in the levels of functional PCI of the 20 patients measured 1 and 3 days after surgery. In this case, method B gave higher values than method A (38% ± 13% versus 29% ± 11% at day 1 and 59% ± 16% versus 43% ± 12% at day 3) (mean ± SD). The level of α1-antitrypsin (α1AT), the second major plasma APC inhibitor, was significantly increased in patients at day 1 and day 3 (133% ± 30% and 190% ± 57%, respectively). Furthermore, there was a positive correlation between the level of α1AT and the normalized difference between the level of functional PCI measured by method B and that measured by method A. Additionally, when normal plasma was supplemented with increasing amounts of purified α1AT, the level of PCI activity measured by method B increased parallel to the increase in α1AT added, but that measured by method A did not. Determination of APC:inhibitor complexes in aliquots of the final mixtures utilized in the PCI assays revealed that the level of APC:α1AT complex increased parallel to the increase in the amount of α1AT added, whereas the APC:PCI complex level remained unchanged. We conclude that current functional PCI assays based on the determination of APC residual activity in plasma are not specific for PCI, are influenced by the level of plasma α1AT and are not reliable for the determination of functional PCI levels in patients with altered levels of α1AT. In contrast, the method based on the determination of the APC:PCI complexes formed following incubation of plasma samples with APC is specific for active PCI and is not influenced for the presence of other APC inhibitors.

Published

1993

18. Activated protein C:α1-antitrypsin (APC:α1AT) complex as a marker for diagnosis of prethrombotic states

Author

Juan Gilabert, Amparo Estellés, Vicente Vicente, Justo Aznar, Lourdes Vazquez, Francisco España, and Sylvia Hendl

Subjects

Proteases, business.industry, Protein C inhibitor, Hematology, medicine.disease, Molecular biology, In vitro, Preeclampsia, Thrombin, Coagulation, Diabetes mellitus, Immunology, medicine, business, Protein C, medicine.drug

Abstract

The purpose of the study was to test whether APC: α 1 AT complex is a useful clinical marker of the activation of coagulation. The rationale for this is that activated protein C may appear in circulation at an early stage of blood coagulation, when subcoagulant amounts of thrombin are formed. Given the relatively higher half-life of APC: α 1 AT as compared to that of thrombin:AT-III (TAT) complexes, we hypothesized that APC: α 1 AT could represent an amplification of the thrombin generated in the first events of coagulation. Using sandwich ELISA's we measured APC: α 1 AT and TAT complexes as well as complexes of AT-III with its target proteases in normal subjects and in several clinical groups of patients prone to thrombotic episodes, including pregnancy, preeclampsia, hemodialysis, gynecological tumors, diabetes and oral contraceptives. APC: α 1 AT complex was significantly increased in all clinical groups as compared to normal subjects and showed relatively higher increases than did TAT and ATM complexes in the majority of the groups studied. There was a significant and positive correlation between APC: α 1 AT and TAT complex levels in the majority of the groups, as well as between TAT and ATM and between APC: α 1 AT and ATM complex levels. We conclude that APC: α 1 AT complex can be used as a sensitive marker of prethrombotic states.

Published

1992

19. Activated protein C levels in obesity and weight loss influence

Author

Amparo Vayá, Silvia Navarro, Amparo Estellés, Francisco España, Eva Solá, Pilar Medina, and Antonio Hernández-Mijares

Subjects

Adult, Male, medicine.medical_specialty, Protein C inhibitor, food.diet, Body Mass Index, food, Thrombin, Weight loss, Internal medicine, Weight Loss, medicine, Humans, Obesity, Endothelial protein C receptor, business.industry, Hematology, Middle Aged, medicine.disease, Peptide Fragments, Very low calorie diet, Endocrinology, Coagulation, Female, Prothrombin, medicine.symptom, business, Protein C, medicine.drug

Abstract

Obesity is associated with a high risk of cardiovascular events. Several haemostatic disturbances which could contribute to this increased risk have been described in obesity; nevertheless, the state of coagulation inhibitors has been scarcely studied in these patients. The aim of the present study was to compare activated protein C levels in obese patients and in a control group, and to evaluate the effect of weight loss. In 67 severe or morbid obese patients, an evaluation was performed at baseline and 3 months after diet. The same determinations were performed in 67 healthy volunteers with normal body weight. We also quantified the levels of protein C and prothrombin fragment 1 + 2. Obese patients showed significantly higher levels of activated protein C, protein C and fragment 1 + 2. No correlation was found between activated protein C and fragment 1 + 2 levels in obese patients. After three months of diet, a significant decrease in activated protein C and fragment 1 + 2 was observed. In conclusion, activated protein C levels are increased in obese patients, but only a minor fraction of this increase may be explained by the higher thrombin generation and C protein levels. Activated protein C levels decrease with weight loss, due in part to a thrombin generation reduction.

Published

2008

20. Anti-coagulant aptamers

Author

Subash C. B. Gopinath

Subjects

business.industry, Aptamer, SELEX Aptamer Technique, Anticoagulants, Hematology, Computational biology, Factor VIIa, Aptamers, Nucleotide, Antithrombins, Factor IX, Coagulation cascade, Immunology, Medicine, Animals, Humans, business, Aptamer Technology, Blood Coagulation, Protein C Inhibitor

Abstract

In the past decade development of aptamer technology is poised into several fields with various clinical applications. With this progress, aptamer based anti-coagulant agents are evolved and continuing their applications with clinical trials. At present several anti-coagulant aptamers are available against different proteins from blood coagulation cascade. In this review, the mechanism and functions of anti-coagulant aptamers, as an alternate candidate to other available anti-coagulant agents are discussed.

Published

2007

21. Early identification of acute myocardial infarction by activated protein C--protein C inhibitor complex

Author

Johan Stenflo, Pallonji Bhiladvala, Karin Strandberg, and Johan Holm

Subjects

Adult, Male, Acute coronary syndrome, medicine.medical_specialty, Time Factors, Protein C inhibitor, Myocardial Infarction, Sensitivity and Specificity, Electrocardiography, Coronary thrombosis, Risk Factors, Internal medicine, Troponin I, medicine, Humans, Fluorometry, cardiovascular diseases, Myocardial infarction, Creatine Kinase, Aged, Protein C Inhibitor, Aged, 80 and over, biology, business.industry, ST elevation, Hematology, Middle Aged, medicine.disease, Troponin, Thrombosis, Evaluation Studies as Topic, biology.protein, Cardiology, Biological Assay, Female, Blood Coagulation Tests, business, Protein C

Abstract

Introduction: Increased coagulation activity due to coronary thrombosis in a ruptured plaque should result in activation of the protein C anticoagulant system with formation of complexes between activated protein C (APC) and,the protein C inhibitor (PCI), which reflects coagulation activity. We hypothesized that elevated APC-PCI concentration might allow earlier detection of ongoing myocardial infarction than traditional biochemical markers. We have evaluated a newly devised immunofluorimetric assay for measuring plasma concentration of APC-PCI complexes among patients with suspected acute coronary syndrome. Materials and methods: Blood samples were taken from 340 patients (median 71 years, range 31-97) with suspected acute coronary syndrome at first presentation in the emergency department. Electrocardiogram was recorded and APC PCI, Troponin I and Creatine kinase-MB concentrations were repeatedly measured 3 times at 6 h interval. Results: The 74 patients who were eventually diagnosed with myocardial infarction had a higher median level of APC-PCI complex than those Without myocardial damage; 0.27 vs. 0.20 mu g/L (p = 0.001). In a multivariate regression model, APC-PCI level in the fourth quartile (> 0.32 mu g/L) independently predicted myocardial infarction with an odds ratio of 3.7 (95% CI 1.4-9.6, p < 0.01). Conclusion: Early APC-PCI elevation can be detected among patients with a normal first Troponin I and non-ST-elevation myocardial infarction and provides additional risk assessment in acute coronary syndrome. (c) 2005 Published by Elsevier Ltd. (Less)

Published

2005

22. C0069 Association of haplotypes (H) 1 and 3 of the endothelial protein c receptor gene (PROCR) with venous thromboembolism

Author

Pilar Medina, Rogier M. Bertina, Laura Martos, Silvia Navarro, José Antonio Aznar, Amparo Estellés, Amparo Vayá, Yolanda Mira, Francisco España, Fernando Ferrando, and Elena Bonet

Subjects

Endothelial protein C receptor, business.industry, medicine.drug_class, Protein C inhibitor, Anticoagulant, Hematology, Heparin, medicine.disease, Molecular biology, Venous thrombosis, In vivo, Conventional PCI, Medicine, business, Protein C, medicine.drug

Abstract

Background: Activated protein C (APC) is an enzyme with anticoagulant and cytoprotective functions. Accumulative data suggest that the number of situations in which in vivo circulating APC will need to be measured will increase over the next few years. Therefore, the availability of a rapid, sensitive and simple assay for quantifying circulating APC is crucial. Available assays are difficult to apply in routine laboratory. Our previously reported assay required an excessive pre-analytical handling: drawing of blood into two citrate tubes; immediate addition of a fresh APC inhibitor to one tube in order to block complexation of circulating APC to protein C inhibitor (PCI), and of heparin to the other tube to force all circulating APC to bind to PCI, and measurement of APC:PCI complexes in both tubes by ELISA (method A). Here we describe a simplifiedmethod based on the measurement of APC:PCI in a unique blood tube anticoagulated with heparin (method B). Methods: We measured APC levels, with both methods, in 125 plasma samples, 69 from patients with venous thrombosis (VT) and 56 from healthy controls. Results: ThemeanAPC level in the 125 sampleswas 1.06±0.46 ng/ml (method A) and 2.21±0.85 ng/ml (method B). The coefficient of correlation between both methods was r=0.849 (Pb0.001). The mean APC level in the 69 VT patients wase 0.84±0.38 (method A) and 1.80± 0.67 (method B), significantly lower (as previously reported) than those in the 56 controls, 1.33±0.39 and 2.72±0.79, respectively, (Pb0.001). In both groups there was a significant correlation between the levels obtained by the two methods (VT, r=0.772; controls, r=0.777 (Pb0.001). Comment: These results show that both assays are equivalent, and confirm that the APC level is lower in VT patients than in healthy individuals. Therefore, the new simplified assay, which measures the sum of circulating free APC and APC complexed to PCI, may be used to estimate the level of circulating APC, and will allow its use in routine laboratories. (FIS PS09/00610, RECAVA RD06/0014/0004, Prometeo/ 2011/027, y Fundacion para la Investigacion Hospital La Fe; Pilar Medina is a Miguel Servet Researcher, ISCIII CP09/00065).

Published

2012

23. Role of each Asn-linked glycan in the anticoagulant activity of human protein C inhibitor

Author

Wakako Izutani, Hiroyuki Shirono, Kenichi Takahashi, Koji Nishizawa, Junichi Koga, and Mitsugu Fujita

Subjects

Glycan, Glycosylation, Serine Proteinase Inhibitors, biology, Protein C inhibitor, Mutant, Thrombin, Hematology, Kallikrein, Serine, Glutamine, Biochemistry, Amino Acid Substitution, Polysaccharides, medicine, biology.protein, Mutagenesis, Site-Directed, Humans, Kallikreins, Asparagine, Blood Coagulation, Protein C, medicine.drug, Protein C Inhibitor

Abstract

The N-glycosylation site mutants of human protein C inhibitor (PCI; N230S, N243Q, N319Q, N230S/N243Q, and N230S/N319Q) were prepared by amino acid replacement of the asparagine residue with a serine or glutamine residue using site-directed mutagenesis and expressed in the baculovirus/insect cell expression system. To examine the importance of each Asn-linked glycan in the activity of PCI, we compared wtPCI with the mutants of N-glycosylation site(s) in terms of the procoagulant protease-inhibitory and anticoagulant activities. The inhibitory activities of N230S, N319Q, and N230S/N319Q toward human thrombin and plasma kallikrein were significantly increased compared with wtPCI, but those of N243Q and N230S/N243Q were reduced. The inhibitory activity of N230S toward human plasma coagulation was significantly increased compared with wtPCI, and that of N230S/N319Q was also significantly increased compared with N319Q. Furthermore, the procoagulant protease-inhibitory and anticoagulant activities of N230S/N319Q (glycosylated on Asn243 only) compared favorably with those of N230S, and both of the mutants possessed highest activities in the purified mutants. These results suggest that the Asn243-linked glycan in PCI molecule possesses critical roles for its anticoagulant activity in the circulation, and the Asn230-linked glycan down-regulates the activity of PCI.

Published

2002

24. The trimannosyl cores of N-glycans are important for the procoagulant protease-inhibitory activity of urinary protein C inhibitor

Author

Junichi Koga, Koji Nishizawa, Mitsugu Fujita, and Wakako Izutani

Subjects

Glycan, Glycosylation, Serine Proteinase Inhibitors, Protein C inhibitor, medicine.medical_treatment, Molecular Sequence Data, Mannose, chemistry.chemical_compound, Thrombin, Exoglycosidase, medicine, Humans, Amino Acid Sequence, Glycoproteins, Protein C Inhibitor, chemistry.chemical_classification, Protease, Binding Sites, biology, Hematology, Molecular biology, carbohydrates (lipids), chemistry, Biochemistry, Carbohydrate Sequence, biology.protein, Kallikreins, Glycoprotein, Trisaccharides, medicine.drug

Abstract

We investigated the relationship between the procoagulant protease-inhibitory activity and the N-glycan structures in urinary protein C inhibitor (uPCI) by sequential exoglycosidase digestions based on the N-glycan structures elucidated in this report. uPCI was glycosylated on the three potential N-glycosylation sites, asparagines 230, 243 and 319 (N230, N243 and N319) in the molecule and had four biantennary complex type sugar chains. The inhibitory activities of uPCI toward thrombin and plasma kallikrein were little changed by the sequential removal of N-acetylneuraminic acid and galactose residues from the termini and N-acetylglucosamine residues from the branches of the N-glycans. However, the inhibitory activities were markedly decreased by further removing alpha-mannose residues from the trimannosyl cores of the N-glycans. These results suggest that the trimannosyl cores of N-glycans are important for uPCI to inhibit the procoagulant protease.

Published

2001

25. Activation of the protein C pathway in acute sepsis

Author

Amparo Estellés, Jaime Sánchez-Cuenca, Justo Aznar, Francisco España, Vicente Vicente, Isabel Zuazu, and Antonio Alcaraz

Subjects

Adult, Male, medicine.medical_specialty, Time Factors, Adolescent, Protein C inhibitor, Antithrombin III, Fibrinogen, Fibrin, Sepsis, Fibrin Fibrinogen Degradation Products, Thrombin, In vivo, Internal medicine, medicine, Humans, cardiovascular diseases, Blood Coagulation, Aged, biology, business.industry, Platelet Count, Hematology, Middle Aged, medicine.disease, Blood Coagulation Factors, Enzyme Activation, Endocrinology, alpha 1-Antitrypsin, Immunology, Conventional PCI, Acute Disease, biology.protein, Female, Kallikreins, business, Protein C, medicine.drug, Peptide Hydrolases

Abstract

To obtain quantitative information on the in vivo activation of the protein C system during the acute phase of sepsis, several components of the protein C pathway were studied in 18 patients. Blood samples were obtained one day after diagnosis (day 1) and, in 11 patients, also on the fourth and tenth days after diagnosis (days 4 and 10). On day 1, patients showed laboratory signs of haemostatic alterations such as positive fibrinogen/fibrin degradation products, and increased thrombin:antithrombin-III (TAT) complex levels. Compared with the control group, patients on day 1 had significantly decreased (p0.001) antigenic protein C (69 +/- 28%) and protein C inhibitor (PCI) (33 +/- 22%) whereas a significant increase in the levels of activated protein C (APC) complexed with alpha 1-antitrypsin (alpha 1AT) (APC:alpha 1AT, 26 +/- 15 ng/mL) and APC:PCI complex (3.0 +/- 2.0 ng/mL), and in the level of plasma kallikrein (KK) complexes with PCI (KK:PCI) (31 +/- 22 ng/mL) was observed. There was a positive correlation between APC:alpha 1AT and TAT complex levels (r = 0.597, p = 0.009). In the follow-up a trend toward normal values in antigenic protein C and PCI, and in APC:PCI and KK:PCI complex levels was found. However, PCI remained significantly decreased compared to normal values. C4b-binding protein, alpha 1AT, and TAT and APC:alpha 1AT complexes did not show any significant variations during the course of the disease, suggesting the contribution of the inflammatory and haemostatic responses, in spite of the good recovery of the patients. This study shows that in the course of sepsis, patients experience a generalized activation of the protein C pathway which was more prominent on day 1, resulting in the consumption of protein C and PCI and in the increase of APC:inhibitor complexes. Moreover, these data provide further evidence that KK:PCI circulating complexes occur in vivo.

Published

1995

26. C0068 Haplotypes of the endothelial protein C receptor gene and circulating protein C levels

Author

José A. Aznar, Elena Bonet, Francisco España, Esther Zorio, Laura Martos, Miguel A. Arnau, Ana Osa, Amparo Estellés, Joaquín Rueda, Silvia Navarro, Pilar Medina, and Rogier M. Bertina

Subjects

Endothelial protein C receptor, Chemistry, medicine.drug_class, Protein C inhibitor, LRP1B, Anticoagulant, Hematology, Heparin, Molecular biology, In vivo, Conventional PCI, medicine, Protein C, medicine.drug

Abstract

Background: Activated protein C (APC) is an enzyme with anticoagulant and cytoprotective functions. Accumulative data suggest that the number of situations in which in vivo circulating APC will need to be measured will increase over the next few years. Therefore, the availability of a rapid, sensitive and simple assay for quantifying circulating APC is crucial. Available assays are difficult to apply in routine laboratory. Our previously reported assay required an excessive pre-analytical handling: drawing of blood into two citrate tubes; immediate addition of a fresh APC inhibitor to one tube in order to block complexation of circulating APC to protein C inhibitor (PCI), and of heparin to the other tube to force all circulating APC to bind to PCI, and measurement of APC:PCI complexes in both tubes by ELISA (method A). Here we describe a simplifiedmethod based on the measurement of APC:PCI in a unique blood tube anticoagulated with heparin (method B). Methods: We measured APC levels, with both methods, in 125 plasma samples, 69 from patients with venous thrombosis (VT) and 56 from healthy controls. Results: ThemeanAPC level in the 125 sampleswas 1.06±0.46 ng/ml (method A) and 2.21±0.85 ng/ml (method B). The coefficient of correlation between both methods was r=0.849 (Pb0.001). The mean APC level in the 69 VT patients wase 0.84±0.38 (method A) and 1.80± 0.67 (method B), significantly lower (as previously reported) than those in the 56 controls, 1.33±0.39 and 2.72±0.79, respectively, (Pb0.001). In both groups there was a significant correlation between the levels obtained by the two methods (VT, r=0.772; controls, r=0.777 (Pb0.001). Comment: These results show that both assays are equivalent, and confirm that the APC level is lower in VT patients than in healthy individuals. Therefore, the new simplified assay, which measures the sum of circulating free APC and APC complexed to PCI, may be used to estimate the level of circulating APC, and will allow its use in routine laboratories. (FIS PS09/00610, RECAVA RD06/0014/0004, Prometeo/ 2011/027, y Fundacion para la Investigacion Hospital La Fe; Pilar Medina is a Miguel Servet Researcher, ISCIII CP09/00065).

Published

2012

27. Functionally active protein C inhibitor/plasminogen activator inhibitor-3 (PCI/PAI-3) is secreted in seminal vesicles, occurs at high concentrations in human seminal plasma and complexes with prostate-specific antigen

Author

Antonio Cabo, Justo Aznar, Amparo Estellés, Francisco España, Juan Gilabert, and Alberto Romeu

Subjects

Male, medicine.medical_specialty, Protein C inhibitor, Semen, Biology, Urine, Thrombin, Antigens, Neoplasm, Internal medicine, Blood plasma, medicine, Humans, cardiovascular diseases, Saliva, Protein C Inhibitor, Seminal Vesicles, Hematology, Kallikrein, Blood Proteins, Prostate-Specific Antigen, Amniotic Fluid, surgical procedures, operative, Endocrinology, Conventional PCI, Female, therapeutics, Plasminogen activator, Protein C, medicine.drug, Protein Binding

Abstract

Protein C inhibitor (PCI) is a heparin-dependent serpin present in a native form in plasma at concentrations of 5 micrograms/mL. In vitro, PCI inhibits activated protein C (APC), thrombin, plasma kallikrein (KK) and urokinase-(uPA) and tissue-type plasminogen activator (tPA), and we have shown in vivo inhibition of APC, uPA and KK by PCI. In order to further characterize the physiological role of PCI, we have measured the level of PCI in several biological fluids. PCI antigen was assayed by ELISA and PCI activity was measured by its capability to form complexes with APC in the presence of heparin. Seminal plasma from voluntary donors had PCI levels (160 +/- 20 micrograms/mL, mean +/- SD) about 30 or 40 times higher than those found in blood plasma. Patients under a fertilization program had significantly reduced PCI seminal levels (110 +/- 35 micrograms/mL). Seminal plasma PCI retained about 45% of its activity immediately after ejaculation, and the activity rapidly decreased following incubation of seminal plasma at 37 degrees C, in parallel with the appearance of complexes of PCI with prostate-specific antigen (PSA). PCI was present in seminal vesicle secretion, obtained by autopsy, at concentration similar to that observed in semen, was mostly active and was not inactivated by incubation of secretion at 37 degrees C. The mean functional and antigen levels of PCI in urine from normal donors were 0.58 and 0.25 micrograms/mL, respectively, whereas in saliva these levels were 20 and 0.8 ng/mL, respectively. Amniotic fluid contained PCI antigen levels of 2.1 +/- 0.2 microgram/mL. These results show that PCI is secreted in the seminal vesicles in a functional form, and suggest that PSA, a major secretory component of the prostate, is responsible for its inactivation. They also suggest a physiological role of PCI in reproduction, and show that PCI is present in various biological fluids.

Published

1991

28. Determination of plasma protein C inhibitor and of two activated protein C-inhibitor complexes in normals and in patients with intravascular coagulation and thrombotic disease

Author

Vicente Vicente, Dolores Tabernero, John H. Griffin, Francisco España, and Inge Scharrer

Subjects

Pathology, medicine.medical_specialty, Serine Proteinase Inhibitors, Protein C inhibitor, Enzyme-Linked Immunosorbent Assay, Gastroenterology, Internal medicine, Blood plasma, medicine, Humans, cardiovascular diseases, Protein C Inhibitor, Disseminated intravascular coagulation, business.industry, Thrombosis, Hematology, Heparin, Blood Proteins, Disseminated Intravascular Coagulation, Thrombophlebitis, medicine.disease, Blood proteins, Kinetics, Coagulation, alpha 1-Antitrypsin, Conventional PCI, business, Protein C, medicine.drug

Abstract

We developed an ELISA to quantitate complexes of activated protein C (APC) with a major plasma APC inhibitor, alpha 1-antitrypsin (alpha 1AT) in human plasma based on the sandwich principle using two different antibodies directed towards protein C and alpha 1AT, respectively. This ELISA test was specific for APC:alpha 1AT complexes and sensitive to greater than or equal to 150 pg complex. Fifty-one of 56 healthy donors had APC:alpha 1AT complex levels above the detection limit (3 ng/ml) ranging from 4 to 14 ng/ml (mean value +/- SD: 7.6 +/- 2.5 ng/ml). Patients (n = 10) with disseminated intravascular coagulation (DIC) had detectable levels of APC:alpha 1AT complex ranging from 21 to 125 ng/ml (median: 69 ng/ml). Complexes of APC with plasma protein C inhibitor (PCI) were also measured using an ELISA sandwich assay. None of the 30 healthy donors had detectable levels (greater than or equal to 5 ng/ml) of APC:PCI complex, and plasma samples from 9 of 10 DIC patients had detectable concentrations of APC:PCI complex ranging from 10 to 63 ng/ml (median: 22 ng/ml). APC:alpha 1AT complex was detected in 25 of 26 patients with deep venous thrombosis (DVT), with levels ranging from 5 to 136 ng/ml (median: 23 ng/ml), whereas APC:PCI was detected in only 6 DVT patients, with levels between 11 and 105 ng/ml. PCI antigen levels in 70 normals ranged from 56 to 175% (mean +/- SD: 99.1% +/- 24.2%). PCI antigen levels were decreased in DIC patients, in patients with cerebral arterial thrombosis, and in DVT patients undergoing heparin therapy, but not in patients with myocardial infarction. PCI antigen levels were decreased much further in DVT patients receiving heparin compared to those not receiving heparin, showing that heparin therapy is associated with a decrease in PCI levels. The detection in normal subjects and in thrombotic patients of circulating APC:inhibitor complexes supports the view that the protein C pathway is activated during DIC and DVT. Moreover, it emphasizes that both PCI and alpha 1AT are physiologic inhibitors of APC. Thus, measurement of APC complexes may provide sensitive parameters for specific detection of activation of the clotting and protein C pathways.

Published

1990

29. Host protein C inhibitor inhibits tumor growth, but promotes tumor metastasis, which is closely correlated with hypercoagulability.

Author

Akita N, Ma N, Okamoto T, Asanuma K, Yoshida K, Nishioka J, Shimaoka M, Suzuki K, and Hayashi T

Subjects

Animals, Female, Humans, Immunoenzyme Techniques, Immunohistochemistry, Male, Melanoma, Experimental, Mice, Mice, Inbred C57BL, Mice, Transgenic, Neoplasm Metastasis, Neoplasm Transplantation, Protein C Inhibitor chemistry, RNA analysis, Thrombomodulin chemistry, Time Factors, Coagulants chemistry, Lung Neoplasms drug therapy, Protein C antagonists & inhibitors, Protein C Inhibitor blood, Thrombophilia blood

Abstract

Introduction: Protein C inhibitor (PCI), a member of the serine protease inhibitor family, is expressed in various human tissues, including liver and kidneys. In the plasma, PCI physiologically inhibits an anticoagulant serine protease, activated protein C (APC). PCI expressed by cancer cells suppresses tumor invasion by inhibiting urokinase-type plasminogen activator, and inhibits tumor growth and metastasis, which are independent of its protease-inhibitory activity. In the present study, we clarified the effects of host PCI on growth and metastasis of B16 melanoma (B16) cells by comparing between wild-type mice and mice transgenic for human PCI gene (hPCI-TG), which have a tissue distribution of PCI similar to that observed in humans., Materials and Methods: Growth of intracutaneously-injected B16 cells was evaluated by measuring the tumor volume, and metastatic behavior of intravenously-injected B16 cells by counting the number of metastatic lung nodules., Results: Growth of intracutaneously injected B16 cells was significantly faster in wild-type mice than in hPCI-TG mice; however, hPCI-TG mice developed more metastatic nodules of B16 cells in the lungs. Immunohistochemical analysis using anti-mouse fibrinogen antibody revealed more fibrin deposition in the lung in hPCI-TG mice than in wild-type mice. Furthermore, the more invasive behavior observed in hPCI-TG mice was reduced by rabbit anti-human PCI IgG, APC, or soluble TM administration for 3 consecutive days including the day that B16 cells were injected., Conclusions: Our results suggest that like PCI expressed in tumor cells, host PCI also inhibits tumor growth, but host PCI promotes tumor metastasis via its procoagulant properties., (Copyright © 2015 Elsevier Ltd. All rights reserved.)

Published

2015

30. An elisa for the measurement of complexes between urokinase plasminogen activator and protein C inhibitor

Author

Francisco España, Justo Aznar, Amparo Estellés, Juan Gilabert, and Sylvia Hendl

Subjects

Urokinase receptor, Chemistry, Urokinase Plasminogen Activator, Protein C inhibitor, Hematology, Molecular biology

Published

1992

31. Protein C inhibitor: Purification and proteinase reactivity

Author

B.Gail Macik, Frank C. Church, and Charlotte W. Pratt

Subjects

biology, Heparin, Chemistry, Protein C inhibitor, Blood Proteins, Hematology, Molecular biology, Kinetics, Thrombin, Biochemistry, In vivo, Protein A/G, medicine, biology.protein, Humans, Protease Inhibitors, Protein G, Polyacrylamide gel electrophoresis, Protein C, Protein C Inhibitor, medicine.drug

Abstract

Protein C inhibitor was purified from human plasma by a modification of a published procedure (Suzuki, K., Nishioka, J., and Hashimoto, S. J. Biol. Chem. 258, 163–168, 1983). Approximately 1 mg of pure protein was obtained from 1 L plasma, a yield of about 17%. The protein C inhibitor preparation did not lose activity over 4 weeks at 4°C. Second order rate constants were measured for the inhibition of activated protein C, thrombin, and urokinase, and bimolecular complexes of protein C inhibitor with activated protein C and thrombin were visualized by denaturing polyacrylamide gel electrophoresis. Heparin accelerated the inhibition of the three proteinases in a manner consistent with a template mechanism. Plasma or pure protein C inhibitor (at the same concentration) showed the same effect of heparin on activated protein C inhibition, indicating that protein C inhibitor accounts for all the heparin-dependent inhibition of activated protein C in vivo.

Published

1989

32. Specificity of sulfated polysaccharides to accelerate the inhibition of activated protein C by protein C inhibitor

Author

Kaoru Takahashi, Yoshiaki Kazama, Nobuo Sakuragawa, Masahiro Niwa, Takehiko Koide, and Ryoichi Yamagishi

Subjects

chemistry.chemical_classification, Chemistry, Protein C inhibitor, Dextran Sulfate, Dextrans, Hematology, Heparin, Pentosan polysulfate, Polysaccharide, Enzyme Activation, Molecular Weight, Kinetics, chemistry.chemical_compound, Dextran, Biochemistry, Polysaccharides, medicine, Humans, Chondroitin, Sulfate, Protein C, medicine.drug

Abstract

The ability of various sulfated polysaccharides to activate protein C inhibitor (PCI) and the effect of molecular weight (Mr) and sulfur content of dextran sulfates were investigated. Besides dextran sulfate, highly sulfated polysaccharides such as chondroitin polysulfates 1 and 5, and pentosan polysulfate were more active than heparin in enhancing the activated protein C inhibition by PCI. The molecular weight and the sulfur content of dextran sulfate were critical for the second-order rate constant of the reaction and for the optimal concentration of the polysaccharide, respectively. These results suggest that the carboxyl groups of polysaccharides are not necessarily required, but some sulfate groups within polymers may play a critical role in the interaction with PCI.

Published

1987

33. Determination of functional and antigenic protein C inhibitor and its complexes with activated protein C in plasma by ELISA's

Author

Francisco España and John H. Griffin

Subjects

Male, Chromatography, biology, Chemistry, medicine.drug_class, Protein C inhibitor, Enzyme-Linked Immunosorbent Assay, Blood Proteins, Hematology, Monoclonal antibody, Epitope, surgical procedures, operative, Antigen, Conventional PCI, Blood plasma, medicine, biology.protein, Humans, cardiovascular diseases, Antibody, therapeutics, Protein C, Protein C Inhibitor, medicine.drug

Abstract

Enzyme-linked immunosorbent assays (ELISA's) were developed for the measurement of protein C inhibitor (PCI) antigen and activity and for its complexes with activated protein C (APC) in plasma. For PCI activity and antigen, APC or anti-PCI, respectively, was immobilized to microtiter plates and PCI bound was detected with labelled anti-PCI antibodies. For APC:PCI complexes, two different antibodies directed against protein C and PCI were used. The assays for PCI were calibrated with pooled normal human plasma (NHP) and with purified PCI, and for APC:PCI complexes with known concentrations of purified pre-formed complexes added to buffer or to plasma. The lower limit of sensitivity of the PCI activity and antigen assays was 10 ng/ml and 0.5 ng/ml, respectively and for plasma APC:PCI complexes 12 ng/ml. Mean coefficients of variation of 1.5% to 5.8% (intra-assay) and 2.1% to 9.8% (inter-assay) were found for the assays. For PCI antigen, a range of 56% to 162% of the NHP value was obtained in samples from 70 healthy donors (mean +/- SD = 98.6% +/- 23.1%). For PCI activity, the range was 59% to 148% (94.3% +/- 20.2). A good correlation (0.92) was obtained when both assays were compared. Plasma levels of APC:PCI complexes in 30 normals were under the detection limit (less than 12 ng/ml). In plasma samples from 10 patients with disseminated intravascular coagulation (DIC) PCI antigen concentrations were decreased (55.6% +/- 20%) and 8 of the patients had APC-PCI complex levels between 32 and 240 ng/ml (median, 35 ng/ml). After addition of 20 micrograms/ml APC to NHP or to protein C depleted plasma, 6.1 micrograms/ml complexes were recovered after 90 min incubation. Incubation of 10 micrograms/ml APC with NHP in the presence of 10 U/ml heparin yielded 11 micrograms/ml complexes after 90 min, which represent more than 90% of the maximum possible value. Thus, the method should be adequate to study complexes of APC in vivo in clinical conditions in which activation of protein C pathway may occur.

Published

1989

34. Studies on human protein C inhibitor in normal and factor V/VIII deficient plasmas

Author

John H. Griffin and Joyce E. Gardiner

Subjects

biology, Plasma samples, Chemistry, Protein C inhibitor, Factor V, Hematology, Hemophilia A, Biochemistry, Freezing, medicine, biology.protein, Humans, Factor V Deficiency, Protein C, Glycoproteins, medicine.drug

Abstract

Activated protein C is a potent anticoagulant which inactivates Factors V and VIII in plasma. Normal plasma contains an inhibitor of activated protein C. A previous report from our laboratory hypothesized that the absence of this inhibitor in plasmas from patients with combined Factor V/VIII deficiency could be the molecular basis for this disease. This report demonstrates the presence of protein C inhibitor in those Factor V/VIII deficient plasmas originally studied. Freezing and thawing significantly reduced the ability of normal and Factor V/VIII deficient plasmas to inhibit activated protein C. It is suggested that this explains the conflicting literature reports describing functional assays of protein C inhibitor in Factor V/VIII deficient plasma. This observation also emphasizes that extreme care must be used in handling and storing plasma samples that are to be assayed for protein C inhibitor.

Published

1984

35. Further characterization of dextran sulfate as a cofactor of protein C inhibitor

Author

Yoshiaki Kazama, Takehiko Koide, and Nobuo Sakuragawa

Subjects

Stereochemistry, Protein C inhibitor, Antithrombin III, Cofactor, Structure-Activity Relationship, chemistry.chemical_compound, Hyaluronic acid, medicine, Humans, Potency, Structure–activity relationship, Protease Inhibitors, cardiovascular diseases, Sulfate, Protein C Inhibitor, Binding Sites, biology, Heparin, Chemistry, Dextran Sulfate, Dextrans, Blood Proteins, Hematology, Molecular Weight, Kinetics, surgical procedures, operative, Biochemistry, biology.protein, Polyaspartic acid, medicine.drug

Abstract

In the present study, we further investigated the relationship between the potency of dextran sulfate as a cofactor of PCI and its molecular size and/or sulfur content. We also examined the potency of polyaspartic acid and hyaluronic acid to accelerate the APC inhibition by PCI, since both contain many carboxyl groups but no sulfate groups

Published

1989

36. Response of Protein C and Protein C inhibitor to warfarin therapy in patient with combined deficiency of factors V and VIII

Author

Kenneth G. Mann, Koji Suzuki, C. Arkin, Leon W. Hoyer, W. Jensen, M. Gallivan, Murray M. Bern, P. Tracy, and G.L. Davis

Subjects

Adult, medicine.medical_specialty, Factor V Deficiency, Protein C inhibitor, Warfarin therapy, Hemophilia A, Antigen, hemic and lymphatic diseases, Internal medicine, medicine, Humans, In patient, Glycoproteins, Protein C Inhibitor, biology, Chemistry, Warfarin, Factor V, Blood Proteins, Hematology, Endocrinology, biology.protein, Female, Protein C, medicine.drug

Abstract

The role of Protein C in combined factor V/VIII deficiency was examined by reducing the Protein C concentration using warfarin therapy in a patient with the combined deficiency. The factor VIII deficiency was like Hemophilia-A, with deficiency of VIII:C and VIII:C(Ag), but normal VIIIR:Ag and VIIIR:cof. The factor V deficiency was due to loss of the V antigen. During warfarin therapy the Protein C level was reduced, but concentrations of factors V and VIII did not change. Protein C Inhibitor was normal throughout. Thus combined factor V/VIII deficiency is not related to Protein C levels.

Published

1984

37. Purification and characterization of plasma protein C inhibitor

Author

Francisco España, M. Berrettini, and John H. Griffin

Subjects

Gla domain, Serine Proteinase Inhibitors, Chromatography, biology, Plasmin, Chemistry, Protein C inhibitor, Blood Proteins, Hematology, Kallikrein, Heparin, Blood Coagulation Factors, Kinetics, Thrombin, Enzyme inhibitor, medicine, biology.protein, Humans, Partial Thromboplastin Time, cardiovascular diseases, Protein C, Protein C Inhibitor, medicine.drug

Abstract

Plasma protein C inhibitor (PCI) was purified to homogeneity (greater than 95%) with good recovery (greater than 25%) and reproducibility, and the inhibition of a number of blood clotting and fibrinolytic enzymes by purified PCI was studied. PCI inhibited activated protein C (APC), two-chain urokinase (2c-uPA), two-chain tissue plasminogen activator (2c-tPA), thrombin, factor Xa, plasma kallikrein and factor XIa, and this inhibition was accelerated by heparin. The inhibition of each enzyme was accompanied by formation of enzyme inhibitor complexes and by degradation of the inhibitor to lower molecular weight derivatives. Plasma kallikrein and factor XIa cleaved PCI of native Mr = 57,000 into two products with Mr = 54,000 and 52,000 whereas the other enzymes converted the PCI to a product with Mr = 54,000. PCI did not detectably inhibit alpha-factor XIIa or plasmin. Kinetic studies using PCI yielded the following second-order rate constants for inhibition of human APC, 2c-uPA, 2c-tPA, thrombin, factor Xa, kallikrein and factor XIa respectively: 0.65 x 10(4), 0.22 x 10(4), 0.08 x 10(4), 0.61 x 10(4), 2.01 x 10(4), 6.50 x 10(4), and 9.03 x 10(4) M-1s-1 in the absence of heparin and 1.58 x 10(6), 0.43 x 10(6), 0.03 x 10(6), 0.52 x 10(6), 0.09 x 10(6), 0.18 x 10(6) and 0.74 x 10(6) M-1s-1 in the presence of optimal concentrations of heparin. The rate constants for the inhibition of factor XIa and 2c-uPA by PCI suggest a possible role of PCI in the physiologic regulation of these enzymes. The second order rate constants for inhibition of bovine APC and Gla-domainless bovine APC by human PCI were 0.61 x 10(4) and 0.26 x 10(4) M-1s-1 in the absence of heparin and 0.54 x 10(6) and 0.71 x 10(6) M-1s-1 in the presence of heparin, respectively. Calcium ions (0.05 to 4 mM) did not affect these rate constants. The results obtained with normal and Gla-domainless APC indicate that the Gla domain of APC is not required for inactivation by PGI and is not essential for the heparin stimulation of this reaction.

Published

1989

38. Evaluation of two functional assays for protein C inhibitor/plasminogen activator inhibitor-3 activity.

Author

España F, Hendl S, Gilabert J, Estellés A, and Aznar J

Subjects

Amino Acid Sequence, Female, Genital Neoplasms, Female blood, Heparin metabolism, Humans, Male, Molecular Sequence Data, Protein C Inhibitor, Pyrrolidonecarboxylic Acid analogs & derivatives, Risk Factors, Sensitivity and Specificity, Thromboembolism, alpha 1-Antitrypsin analysis, Chromogenic Compounds, Enzyme-Linked Immunosorbent Assay, Oligopeptides, Plasminogen Inactivators analysis, Protein C antagonists & inhibitors

Abstract

Two functional assays for protein C inhibitor (PCI) were evaluated in parallel for the same plasma samples. One assay is specific for active PCI and measures its ability to form complexes with activated protein C (APC) in the presence of heparin (España et al, Thromb Res 64, 309, 1991) (Method A). After incubation of samples with heparin and an excess of APC, the amount of APC:PCI formed is measured by an ELISA. The second functional PCI assay is based on the determination of the residual amidolytic activity of the APC added to the sample. In all cases a good correlation was obtained with both methods. For 20 healthy subjects and 20 patients before surgery, there were no significant between-assay differences in the levels of functional PCI activity. On the other hand, there were significant between-assays differences in the levels of functional PCI of the 20 patients measured 1 and 3 days after surgery. In this case, method B gave higher values than method A (38% +/- 13% versus 29% +/- 11% at day 1 and 59% +/- 16% versus 43% +/- 12% at day 3) (mean +/- SD). The level of alpha 1-antitrypsin (alpha 1 AT), the second major plasma APC inhibitor, was significantly increased in patients at day 1 and day 3 (133% +/- 30% and 190% +/- 57%, respectively). Furthermore, there was a positive correlation between the level of alpha 1AT and the normalized difference between the level of functional PCI measured by method B and that measured by method A. Additionally, when normal plasma was supplemented with increasing amounts of purified alpha 1AT, the level of PCI activity measured by method B increased parallel to the increase in alpha 1AT added, but that measured by method A did not. Determination of APC:inhibitor complexes in aliquots of the final mixtures utilized in the PCI assays revealed that the level of APC:alpha 1AT complex increased parallel to the increase in the amount of alpha 1AT added, whereas the APC:PCI complex level remained unchanged. We conclude that current functional PCI assays based on the determination of APC residual activity in plasma are not specific for PCI, are influenced by the level of plasma alpha 1AT and are not reliable for the determination of functional PCI levels in patients with altered levels of alpha 1AT.(ABSTRACT TRUNCATED AT 400 WORDS)

Published

1993

39. Functionally active protein C inhibitor/plasminogen activator inhibitor-3 (PCI/PAI-3) is secreted in seminal vesicles, occurs at high concentrations in human seminal plasma and complexes with prostate-specific antigen.

Author

España F, Gilabert J, Estellés A, Romeu A, Aznar J, and Cabo A

Subjects

Amniotic Fluid chemistry, Antigens, Neoplasm analysis, Blood Proteins metabolism, Female, Humans, Male, Prostate-Specific Antigen, Protein Binding, Protein C Inhibitor, Saliva chemistry, Urine chemistry, Blood Proteins analysis, Semen chemistry, Seminal Vesicles metabolism

Abstract

Protein C inhibitor (PCI) is a heparin-dependent serpin present in a native form in plasma at concentrations of 5 micrograms/mL. In vitro, PCI inhibits activated protein C (APC), thrombin, plasma kallikrein (KK) and urokinase-(uPA) and tissue-type plasminogen activator (tPA), and we have shown in vivo inhibition of APC, uPA and KK by PCI. In order to further characterize the physiological role of PCI, we have measured the level of PCI in several biological fluids. PCI antigen was assayed by ELISA and PCI activity was measured by its capability to form complexes with APC in the presence of heparin. Seminal plasma from voluntary donors had PCI levels (160 +/- 20 micrograms/mL, mean +/- SD) about 30 or 40 times higher than those found in blood plasma. Patients under a fertilization program had significantly reduced PCI seminal levels (110 +/- 35 micrograms/mL). Seminal plasma PCI retained about 45% of its activity immediately after ejaculation, and the activity rapidly decreased following incubation of seminal plasma at 37 degrees C, in parallel with the appearance of complexes of PCI with prostate-specific antigen (PSA). PCI was present in seminal vesicle secretion, obtained by autopsy, at concentration similar to that observed in semen, was mostly active and was not inactivated by incubation of secretion at 37 degrees C. The mean functional and antigen levels of PCI in urine from normal donors were 0.58 and 0.25 micrograms/mL, respectively, whereas in saliva these levels were 20 and 0.8 ng/mL, respectively. Amniotic fluid contained PCI antigen levels of 2.1 +/- 0.2 microgram/mL. These results show that PCI is secreted in the seminal vesicles in a functional form, and suggest that PSA, a major secretory component of the prostate, is responsible for its inactivation. They also suggest a physiological role of PCI in reproduction, and show that PCI is present in various biological fluids.

Published

1991

40. Fibrinolytic study in a homozygous protein C deficient patient

Author

Francisco España, Justo Aznar, Amparo Estellés, and A. Dasi

Subjects

Male, medicine.medical_specialty, Blood transfusion, medicine.medical_treatment, Protein C inhibitor, Ecchymosis, Tissue plasminogen activator, Gastroenterology, Protein C deficiency, Internal medicine, Thromboembolism, Fibrinolysis, medicine, Coagulopathy, Humans, Blood Transfusion, Glycoproteins, Protein C Inhibitor, business.industry, Homozygote, Anticoagulants, Hematology, Blood Proteins, medicine.disease, Surgery, Tissue Plasminogen Activator, Exercise Test, Female, medicine.symptom, business, Protein C, medicine.drug

Abstract

The fibrinolytic system was evaluated in a patient with homozygous protein C deficiency as well as in several members of his family with a partial deficiency of this protein. Before anticoagulant therapy the patient showed skin lesions which quickly disappeared after administration of fresh plasma. After anticoagulant treatment, the propositus suffered two clinical episodes of "ecchymotic" lesions, which were controlled with fresh plasma. The patient has remained free of new lesions and other clinical episodes up to the present date. The fibrinolytic activity of both the propositus and his family was normal. The patient's father showed adequate release of tissue plasminogen activator after controlled physical exercise. According to clinical and analytical data from our patient and his family, it is suggested that, in spite of the preservation of the fibrinolytic system in this case, a localized deficiency in fibrinolysis could exist in view of the clinical behaviour of the skin lesions described.

Published

1986

41. A functional assay of protein C in human plasma

Author

Inga Marie Nilson, Kyoichi Ikeda, Peter Felding, Gunilla Martinsson, and Christine M. Hickton

Subjects

medicine.medical_specialty, Protein C inhibitor, Radioimmunoassay, Receptors, Cell Surface, Thrombomodulin, Thrombin, Protein C deficiency, Internal medicine, medicine, Animals, Humans, Protease Inhibitors, Glycoproteins, Protein C Inhibitor, medicine.diagnostic_test, Chemistry, Anticoagulants, Hematology, Blood Proteins, Dicoumarol, medicine.disease, Blood Coagulation Factors, Endocrinology, Biochemistry, Cattle, Receptors, Thrombin, Protein C, medicine.drug, Partial thromboplastin time

Abstract

A functional assay for protein C in plasma is described in which barium eluates of plasma are incubated with bovine thrombin and rabbit thrombomodulin to activate protein C. The activated protein C solution is added to an activated partial thromboplastin time (APTT) system containing normal plasma and an APTT reagent (Dade ActinR). The prolongation of coagulation time after recalcification in this system is taken as a measure of the anticoagulant activity of protein C. When expressed as per cent of the value in pooled normal plasma, the results obtained by this method in 34 normal controls and in 3 untreated patients with protein C deficiency were very similar to those obtained by radioimmunoassay of protein C. In 2 patients with protein C deficiency and 23 patients without, all on dicoumarol or warfarin treatment, the anticoagulant activity of protein C was less than its antigen concentration. The day to day analytical coefficient of variation (SD/mean) was 12% at the 100% level (n = 12), and 10% at the 25% level (n = 12).

Published

1986

42. Determination of plasma protein C inhibitor and of two activated protein C-inhibitor complexes in normals and in patients with intravascular coagulation and thrombotic disease.

Author

España F, Vicente V, Tabernero D, Scharrer I, and Griffin JH

Subjects

Enzyme-Linked Immunosorbent Assay, Humans, Kinetics, Protein C Inhibitor, Serine Proteinase Inhibitors blood, Thrombophlebitis blood, alpha 1-Antitrypsin metabolism, Blood Proteins metabolism, Disseminated Intravascular Coagulation blood, Protein C antagonists & inhibitors, Thrombosis blood

Abstract

We developed an ELISA to quantitate complexes of activated protein C (APC) with a major plasma APC inhibitor, alpha 1-antitrypsin (alpha 1AT) in human plasma based on the sandwich principle using two different antibodies directed towards protein C and alpha 1AT, respectively. This ELISA test was specific for APC:alpha 1AT complexes and sensitive to greater than or equal to 150 pg complex. Fifty-one of 56 healthy donors had APC:alpha 1AT complex levels above the detection limit (3 ng/ml) ranging from 4 to 14 ng/ml (mean value +/- SD: 7.6 +/- 2.5 ng/ml). Patients (n = 10) with disseminated intravascular coagulation (DIC) had detectable levels of APC:alpha 1AT complex ranging from 21 to 125 ng/ml (median: 69 ng/ml). Complexes of APC with plasma protein C inhibitor (PCI) were also measured using an ELISA sandwich assay. None of the 30 healthy donors had detectable levels (greater than or equal to 5 ng/ml) of APC:PCI complex, and plasma samples from 9 of 10 DIC patients had detectable concentrations of APC:PCI complex ranging from 10 to 63 ng/ml (median: 22 ng/ml). APC:alpha 1AT complex was detected in 25 of 26 patients with deep venous thrombosis (DVT), with levels ranging from 5 to 136 ng/ml (median: 23 ng/ml), whereas APC:PCI was detected in only 6 DVT patients, with levels between 11 and 105 ng/ml. PCI antigen levels in 70 normals ranged from 56 to 175% (mean +/- SD: 99.1% +/- 24.2%). PCI antigen levels were decreased in DIC patients, in patients with cerebral arterial thrombosis, and in DVT patients undergoing heparin therapy, but not in patients with myocardial infarction. PCI antigen levels were decreased much further in DVT patients receiving heparin compared to those not receiving heparin, showing that heparin therapy is associated with a decrease in PCI levels. The detection in normal subjects and in thrombotic patients of circulating APC:inhibitor complexes supports the view that the protein C pathway is activated during DIC and DVT. Moreover, it emphasizes that both PCI and alpha 1AT are physiologic inhibitors of APC. Thus, measurement of APC complexes may provide sensitive parameters for specific detection of activation of the clotting and protein C pathways.

Published

1990

43. Evidence for a glycine residue at position 316 in human protein C inhibitor.

Author

Meijers JC and Chung DW

Subjects

Amino Acid Sequence, Base Sequence, Humans, Molecular Sequence Data, Oligonucleotides, Polymerase Chain Reaction, Protein C Inhibitor, Sequence Homology, Nucleic Acid, Blood Proteins chemistry, Glycine analysis, Serine Proteinase Inhibitors chemistry

Published

1990

44. Determination of functional and antigenic protein C inhibitor and its complexes with activated protein C in plasma by ELISA's.

Author

España F and Griffin JH

Subjects

Enzyme-Linked Immunosorbent Assay, Humans, Male, Protein C metabolism, Protein C Inhibitor, Blood Proteins analysis, Protein C antagonists & inhibitors

Abstract

Enzyme-linked immunosorbent assays (ELISA's) were developed for the measurement of protein C inhibitor (PCI) antigen and activity and for its complexes with activated protein C (APC) in plasma. For PCI activity and antigen, APC or anti-PCI, respectively, was immobilized to microtiter plates and PCI bound was detected with labelled anti-PCI antibodies. For APC:PCI complexes, two different antibodies directed against protein C and PCI were used. The assays for PCI were calibrated with pooled normal human plasma (NHP) and with purified PCI, and for APC:PCI complexes with known concentrations of purified pre-formed complexes added to buffer or to plasma. The lower limit of sensitivity of the PCI activity and antigen assays was 10 ng/ml and 0.5 ng/ml, respectively and for plasma APC:PCI complexes 12 ng/ml. Mean coefficients of variation of 1.5% to 5.8% (intra-assay) and 2.1% to 9.8% (inter-assay) were found for the assays. For PCI antigen, a range of 56% to 162% of the NHP value was obtained in samples from 70 healthy donors (mean +/- SD = 98.6% +/- 23.1%). For PCI activity, the range was 59% to 148% (94.3% +/- 20.2). A good correlation (0.92) was obtained when both assays were compared. Plasma levels of APC:PCI complexes in 30 normals were under the detection limit (less than 12 ng/ml). In plasma samples from 10 patients with disseminated intravascular coagulation (DIC) PCI antigen concentrations were decreased (55.6% +/- 20%) and 8 of the patients had APC-PCI complex levels between 32 and 240 ng/ml (median, 35 ng/ml). After addition of 20 micrograms/ml APC to NHP or to protein C depleted plasma, 6.1 micrograms/ml complexes were recovered after 90 min incubation. Incubation of 10 micrograms/ml APC with NHP in the presence of 10 U/ml heparin yielded 11 micrograms/ml complexes after 90 min, which represent more than 90% of the maximum possible value. Thus, the method should be adequate to study complexes of APC in vivo in clinical conditions in which activation of protein C pathway may occur.

Published

1989

45. Fibrinolytic study in a homozygous protein C deficient patient.

Author

Aznar J, Dasi A, España F, and Estellés A

Subjects

Anticoagulants pharmacology, Blood Proteins analysis, Blood Transfusion, Ecchymosis blood, Ecchymosis genetics, Exercise Test, Female, Homozygote, Humans, Male, Protein C, Protein C Inhibitor, Thromboembolism blood, Thromboembolism genetics, Tissue Plasminogen Activator analysis, Anticoagulants therapeutic use, Ecchymosis drug therapy, Fibrinolysis, Glycoproteins deficiency, Thromboembolism drug therapy

Abstract

The fibrinolytic system was evaluated in a patient with homozygous protein C deficiency as well as in several members of his family with a partial deficiency of this protein. Before anticoagulant therapy the patient showed skin lesions which quickly disappeared after administration of fresh plasma. After anticoagulant treatment, the propositus suffered two clinical episodes of "ecchymotic" lesions, which were controlled with fresh plasma. The patient has remained free of new lesions and other clinical episodes up to the present date. The fibrinolytic activity of both the propositus and his family was normal. The patient's father showed adequate release of tissue plasminogen activator after controlled physical exercise. According to clinical and analytical data from our patient and his family, it is suggested that, in spite of the preservation of the fibrinolytic system in this case, a localized deficiency in fibrinolysis could exist in view of the clinical behaviour of the skin lesions described.

Published

1986

46. Protein C inhibitor: purification and proteinase reactivity.

Author

Pratt CW, Macik BG, and Church FC

Subjects

Blood Proteins physiology, Heparin pharmacology, Humans, Kinetics, Protein C Inhibitor, Blood Proteins isolation & purification, Protease Inhibitors isolation & purification, Protein C antagonists & inhibitors

Abstract

Protein C inhibitor was purified from human plasma by a modification of a published procedure (Suzuki, K., Nishioka, J., and Hashimoto, S. J. Biol. Chem. 258, 163-168, 1983). Approximately 1 mg of pure protein was obtained from 1 L plasma, a yield of about 17%. The protein C inhibitor preparation did not lose activity over 4 weeks at 4 degrees C. Second order rate constants were measured for the inhibition of activated protein C, thrombin, and urokinase, and bimolecular complexes of protein C inhibitor with activated protein C and thrombin were visualized by denaturing polyacrylamide gel electrophoresis. Heparin accelerated the inhibition of the three proteinases in a manner consistent with a template mechanism. Plasma or pure protein C inhibitor (at the same concentration) showed the same effect of heparin on activated protein C inhibition, indicating that protein C inhibitor accounts for all the heparin-dependent inhibition of activated protein C in vivo.

Published

1989

47. Purification and characterization of plasma protein C inhibitor.

Author

España F, Berrettini M, and Griffin JH

Subjects

Blood Coagulation Factors antagonists & inhibitors, Blood Proteins physiology, Humans, Kinetics, Partial Thromboplastin Time, Protein C Inhibitor, Serine Proteinase Inhibitors, Blood Proteins isolation & purification, Protein C antagonists & inhibitors

Abstract

Plasma protein C inhibitor (PCI) was purified to homogeneity (greater than 95%) with good recovery (greater than 25%) and reproducibility, and the inhibition of a number of blood clotting and fibrinolytic enzymes by purified PCI was studied. PCI inhibited activated protein C (APC), two-chain urokinase (2c-uPA), two-chain tissue plasminogen activator (2c-tPA), thrombin, factor Xa, plasma kallikrein and factor XIa, and this inhibition was accelerated by heparin. The inhibition of each enzyme was accompanied by formation of enzyme inhibitor complexes and by degradation of the inhibitor to lower molecular weight derivatives. Plasma kallikrein and factor XIa cleaved PCI of native Mr = 57,000 into two products with Mr = 54,000 and 52,000 whereas the other enzymes converted the PCI to a product with Mr = 54,000. PCI did not detectably inhibit alpha-factor XIIa or plasmin. Kinetic studies using PCI yielded the following second-order rate constants for inhibition of human APC, 2c-uPA, 2c-tPA, thrombin, factor Xa, kallikrein and factor XIa respectively: 0.65 x 10(4), 0.22 x 10(4), 0.08 x 10(4), 0.61 x 10(4), 2.01 x 10(4), 6.50 x 10(4), and 9.03 x 10(4) M-1s-1 in the absence of heparin and 1.58 x 10(6), 0.43 x 10(6), 0.03 x 10(6), 0.52 x 10(6), 0.09 x 10(6), 0.18 x 10(6) and 0.74 x 10(6) M-1s-1 in the presence of optimal concentrations of heparin. The rate constants for the inhibition of factor XIa and 2c-uPA by PCI suggest a possible role of PCI in the physiologic regulation of these enzymes. The second order rate constants for inhibition of bovine APC and Gla-domainless bovine APC by human PCI were 0.61 x 10(4) and 0.26 x 10(4) M-1s-1 in the absence of heparin and 0.54 x 10(6) and 0.71 x 10(6) M-1s-1 in the presence of heparin, respectively. Calcium ions (0.05 to 4 mM) did not affect these rate constants. The results obtained with normal and Gla-domainless APC indicate that the Gla domain of APC is not required for inactivation by PGI and is not essential for the heparin stimulation of this reaction.

Published

1989

48. A functional assay of protein C in human plasma.

Author

Hickton CM, Felding P, Ikeda K, Martinsson G, and Nilsson IM

Subjects

Animals, Anticoagulants therapeutic use, Blood Proteins isolation & purification, Cattle, Glycoproteins deficiency, Glycoproteins isolation & purification, Humans, Protease Inhibitors isolation & purification, Protein C, Protein C Inhibitor, Radioimmunoassay methods, Receptors, Cell Surface metabolism, Receptors, Thrombin, Thrombin metabolism, Blood Coagulation Factors analysis, Glycoproteins analysis

Abstract

A functional assay for protein C in plasma is described in which barium eluates of plasma are incubated with bovine thrombin and rabbit thrombomodulin to activate protein C. The activated protein C solution is added to an activated partial thromboplastin time (APTT) system containing normal plasma and an APTT reagent (Dade ActinR). The prolongation of coagulation time after recalcification in this system is taken as a measure of the anticoagulant activity of protein C. When expressed as per cent of the value in pooled normal plasma, the results obtained by this method in 34 normal controls and in 3 untreated patients with protein C deficiency were very similar to those obtained by radioimmunoassay of protein C. In 2 patients with protein C deficiency and 23 patients without, all on dicoumarol or warfarin treatment, the anticoagulant activity of protein C was less than its antigen concentration. The day to day analytical coefficient of variation (SD/mean) was 12% at the 100% level (n = 12), and 10% at the 25% level (n = 12).

Published

1986

49. Further characterization of dextran sulfate as a cofactor of protein C inhibitor.

Author

Kazama Y, Koide T, and Sakuragawa N

Subjects

Antithrombin III metabolism, Binding Sites, Dextran Sulfate, Heparin metabolism, Heparin pharmacology, Humans, Kinetics, Molecular Weight, Protein C Inhibitor, Structure-Activity Relationship, Blood Proteins pharmacology, Dextrans pharmacology, Protease Inhibitors pharmacology

Published

1989

50. Response of protein C and protein C inhibitor to warfarin therapy in patient with combined deficiency of Factors V and VIII.

Author

Bern MM, Suzuki K, Mann K, Tracy P, Hoyer L, Jensen W, Gallivan M, Arkin C, and Davis G

Subjects

Adult, Factor V Deficiency blood, Factor V Deficiency complications, Female, Hemophilia A blood, Hemophilia A complications, Humans, Protein C, Protein C Inhibitor, Blood Proteins metabolism, Factor V Deficiency drug therapy, Glycoproteins blood, Hemophilia A drug therapy, Warfarin therapeutic use

Abstract

The role of Protein C in combined factor V/VIII deficiency was examined by reducing the Protein C concentration using warfarin therapy in a patient with the combined deficiency. The factor VIII deficiency was like Hemophilia-A, with deficiency of VIII:C and VIII:C(Ag), but normal VIIIR:Ag and VIIIR:cof. The factor V deficiency was due to loss of the V antigen. During warfarin therapy the Protein C level was reduced, but concentrations of factors V and VIII did not change. Protein C Inhibitor was normal throughout. Thus combined factor V/VIII deficiency is not related to Protein C levels.

Published

1984