Your search keyword '"Protein C Inhibitor"' showing total 219 results

1. Plasma SerpinA5 in conjunction with uterine artery pulsatility index and clinical risk factor for the early prediction of preeclampsia

Author

Yonggang Zhang, Limin Zhao, Hongling Yang, Junzhu Shi, and Yipeng Zhang

Subjects

Embryology, Physiology, Epidemiology, Placenta, Maternal Health, Gastroenterology, Biochemistry, Cohort Studies, Pre-Eclampsia, Pregnancy, Risk Factors, Tandem Mass Spectrometry, Blood plasma, Medicine and Health Sciences, Ultrasonography, Doppler, Color, Enzyme-Linked Immunoassays, Uterine artery, reproductive and urinary physiology, Chromatography, High Pressure Liquid, Protein C Inhibitor, Multidisciplinary, Ultrasound, Obstetrics and Gynecology, Blood proteins, Body Fluids, Trophoblasts, Uterine Artery, Blood, Area Under Curve, Medicine, Biomarker (medicine), Female, Anatomy, Cohort study, Research Article, Adult, medicine.medical_specialty, Science, Enzyme-Linked Immunosorbent Assay, Research and Analysis Methods, Sensitivity and Specificity, Blood Plasma, Preeclampsia, Internal medicine, medicine.artery, medicine, Humans, Immunoassays, Immunohistochemistry Techniques, Plasma Proteins, business.industry, Biology and Life Sciences, Proteins, medicine.disease, Pregnancy Complications, Histochemistry and Cytochemistry Techniques, Pregnancy Trimester, First, Early Diagnosis, ROC Curve, Medical Risk Factors, Immunologic Techniques, Women's Health, Blastocysts, business, Biomarkers, Developmental Biology

Abstract

Object This study aimed to combine plasma protein SerpinA5 with uterine artery doppler ultrasound and clinical risk factor during the first trimester for prediction of preeclampsia. Methods and materials This study was a nested cohort study and was divided into the screening set and developing set. The plasma was collected during the first trimester (11+0–13+6 weeks), at the same time, UtA-PI was detected and recorded with four-dimensional color Doppler ultrasound. These pregnancies were followed up until after delivery. The plasma proteins were examined using ultra-performance liquid chromatography–mass spectrometry (UPLC-MS) and enzyme linked immunosorbent assay (ELISA). Placental samples preserved after delivery were analysed by immunohistochemistry. Clinical risk factors were obtained from medical records or antenatal questionnaires. Upregulation or downregulation of SerpinA5 expression in TEV-1 cells was performed to investigate the role of SerpinA5 in trophoblasts invasion. Results We demonstrated that SerpinA5 levels were greater not only in preeclampsia placental tissue but also in plasma (both p Conclusion These findings showed that placenta-derived plasma SerpinA5 may be a novel biomarker for preeclampsia, which together with uterine artery Doppler ultrasound and clinical risk factor can more effectively predict preeclampsia.

Published

2021

2. Protein C Inhibitor (PCI) Binds to Phosphatidylserine Exposing Cells with Implications in the Phagocytosis of Apoptotic Cells and Activated Platelets.

Author

Rieger, Daniela, Assinger, Alice, Einfinger, Katrin, Sokolikova, Barbora, and Geiger, Margarethe

Subjects

*PROTEIN C inhibitor, *PHOSPHATIDYLSERINE synthase, *PHAGOCYTOSIS, *APOPTOSIS, *ENZYME activation, *HEMOSTASIS

Abstract

Protein C Inhibitor (PCI) is a secreted serine protease inhibitor, belonging to the family of serpins. In addition to activated protein C PCI inactivates several other proteases of the coagulation and fibrinolytic systems, suggesting a regulatory role in hemostasis. Glycosaminoglycans and certain negatively charged phospholipids, like phosphatidylserine, bind to PCI and modulate its activity. Phosphatidylerine (PS) is exposed on the surface of apoptotic cells and known as a phagocytosis marker. We hypothesized that PCI might bind to PS exposed on apoptotic cells and thereby influence their removal by phagocytosis. Using Jurkat T-lymphocytes and U937 myeloid cells, we show here that PCI binds to apoptotic cells to a similar extent at the same sites as Annexin V, but in a different manner as compared to live cells (defined spots on ∼10–30% of cells). PCI dose dependently decreased phagocytosis of apoptotic Jurkat cells by U937 macrophages. Moreover, the phagocytosis of PS exposing, activated platelets by human blood derived monocytes declined in the presence of PCI. In U937 cells the expression of PCI as well as the surface binding of PCI increased with time of phorbol ester treatment/macrophage differentiation. The results of this study suggest a role of PCI not only for the function and/or maturation of macrophages, but also as a negative regulator of apoptotic cell and activated platelets removal. [ABSTRACT FROM AUTHOR]

Published

2014

3. Inhibition profiles of human tissue kallikreins by serine protease inhibitors.

Author

Luo, Liu-Ying and Jiang, Weiping

Subjects

*BIOCHEMISTRY, *BIOMARKERS, *CANCER, *SERINE proteinase inhibitors, *ENZYME regulation

Abstract

Accumulated evidence has shown that human tissue kallikreins (hKs), a group of 15 homologous secreted serine proteases, are novel cancer biomarkers. We report here the inhibition profiles of selected hKs, including hK5, hK7, hK8, hK11, hK12, hK13, and hK14, by several common serine protease inhibitors (serpins) found in plasma. The association constants for the binding of serpins to kallikreins were determined and compared. Protein C inhibitor was found to be the fastest-binding serpin for most of these hKs. α2-Antiplasmin, α1-antichymotrypsin, and α1-antitrypsin also showed rapid inhibition of certain hKs. Kallistatin exhibited fast inhibition only with hK7. Our data demonstrate that these hKs are specifically regulated by certain serpins and their distinct inhibition profiles will be valuable aids in various aspects of kallikrein research. [ABSTRACT FROM AUTHOR]

Published

2006

4. Design and characterization of an APC-specific serpin for the treatment of hemophilia

Author

Ty E. Adams, Stéphanie G. I. Polderdijk, Trevor Baglin, Rodney M. Camire, Lacramioara Ivanciu, and James A. Huntington

Subjects

0301 basic medicine, Protein C inhibitor, Immunology, 030204 cardiovascular system & hematology, Serpin, Hemophilia A, Hemophilia B, Biochemistry, Fibrin, Thrombosis and Hemostasis, Mice, 03 medical and health sciences, 0302 clinical medicine, Thrombin, In vivo, Hemarthrosis, Factor V Leiden, medicine, Animals, Humans, Serpins, Protein C Inhibitor, biology, business.industry, Cell Biology, Hematology, medicine.disease, Disease Models, Animal, 030104 developmental biology, Drug Design, Hemostasis, biology.protein, Cancer research, Electrophoresis, Polyacrylamide Gel, business, Protein C, medicine.drug

Abstract

Hemophilia is a bleeding disorder caused by deficiency in factors VIII or IX, the two components of the intrinsic Xase complex. Treatment with replacement factor can lead to the development of inhibitory antibodies, requiring the use of bypassing agents such as factor VIIa and factor concentrates. An alternative approach to bypass the Xase complex is to inhibit endogenous anticoagulant activities. Activated protein C (APC) breaks down the complex that produces thrombin by proteolytically inactivating factor Va. Defects in this mechanism (eg, factor V Leiden) are associated with thrombosis but result in less severe bleeding when co-inherited with hemophilia. Selective inhibition of APC might therefore be effective for the treatment of hemophilia. The endogenous inhibitors of APC are members of the serpin family: protein C inhibitor (PCI) and α1-antitrypsin (α1AT); however, both exhibit poor reactivity and selectivity for APC. We mutated residues in and around the scissile P1-P1' bond in PCI and α1AT, resulting in serpins with the desired specificity profile. The lead candidate was shown to promote thrombin generation in vitro and to restore fibrin and platelet deposition in an intravital laser injury model in hemophilia B mice. The power of targeting APC was further demonstrated by the complete normalization of bleeding after a severe tail clip injury in these mice. These results demonstrate that the protein C anticoagulant system can be successfully targeted by engineered serpins and that administration of such agents is effective at restoring hemostasis in vivo.

Published

2017

5. Activated protein C assays: A review

Author

Álvaro Fernández-Pardo, Francisco España, Julia Oto, Manuel Miralles, Emma Plana, Silvia Navarro, and Pilar Medina

Subjects

0301 basic medicine, medicine.drug_class, Protein C inhibitor, Clinical Biochemistry, Pharmacology, Biochemistry, law.invention, 03 medical and health sciences, 0302 clinical medicine, Thrombin, law, medicine, Humans, Disseminated intravascular coagulation, business.industry, Biochemistry (medical), Anticoagulant, General Medicine, medicine.disease, Clinical trial, 030104 developmental biology, 030220 oncology & carcinogenesis, Recombinant DNA, business, Function (biology), Protein C, medicine.drug

Abstract

Activated protein C (APC) acts as an "on demand" anticoagulant, reducing thrombin formation. Reduced plasma levels of APC or protein C (PC) are associated with an increased risk of venous thromboembolism. APC also displays cytoprotective functions and its therapeutic use has been evaluated in severe sepsis and is under evaluation in several diseases with an important inflammatory component. In addition, different studies have revealed a potential role of PC/APC in disorders such as obesity, pneumonia, disseminated intravascular coagulation, Alzheimer, stroke, etc. Accordingly, the therapeutic value of different recombinant APC molecules that lack anticoagulant activity but retain the cytoprotective function is being tested in clinical trials for some of these diseases. Therefore, an available method to measure circulating APC in plasma is of great interests. About 16 different methods for the quantification of APC have been reported. Here, we will review the available assays, highlighting their advantages and disadvantages as well as their different stages of implementation and the most appropriate use for each method, including their potential clinical usefulness.

Published

2019

6. Revisiting the activated protein C-protein S-thrombomodulin ternary pathway: Impact of new understanding on its laboratory investigation

Author

Jean Amiral and Jerard Seghatchian

Subjects

Protein C inhibitor, Thrombomodulin, 030204 cardiovascular system & hematology, Protein S, 03 medical and health sciences, 0302 clinical medicine, Thrombin, medicine, Animals, Humans, Blood Coagulation, biology, Chemistry, Factor V, Hematology, Complement system, Coagulation, Biochemistry, biology.protein, Protein C, 030215 immunology, medicine.drug, Signal Transduction

Abstract

Although suspected conceptually in the 60 s, Protein C and Protein S activities in hemostasis were investigated and reported from the mid-80 s, followed by the discovery of Thrombomodulin, an endothelial cell membrane associated protein, playing the most important heamostatic role. These 3 proteins act in regulating thrombogenesis and protecting against thrombo-embolic events. When blood is activated, any trace of circulating thrombin is captured by Thrombomodulin in the microcirculation, making thrombin become an anticoagulant through its capacity to activate Protein C to Activated Protein C, which operates as a sentinel in blood coagulation, in the form of a complex with free Protein S, to block any new blood activation site, and more especially circulating activated Factors V and VIII. Protein S not only acts as the Activated Protein C cofactor, but also as the cofactor of Tissue Factor Pathway Inhibitor. In addition, it has some functions in the complement pathway through its binding to C4b-BP. Another capability of activated protein C is to lower fibrinolytic activity, as the Activated Protein C Inhibitor is also known as Plasminogen Activator Inhibitor 3. The Protein C-Protein S system becomes less efficient in the presence of mutated Factor V (Factor V-Leiden or other variants), which is resistant to its inactivating effect. Other pathologies linked to this system concern the development of allo- or auto-antibodies to Protein S or to thrombin, which can generate severe thrombotic complications in affected patients. Some antithrombotic drugs have originated from this regulatory system. Protein C or Protein S concentrates are used for treating deficient patients. Activated Protein C (especially in patients with sepsis) or Thrombomodulin are proposed as antithrombotic medications. Most importantly, congenital or acquired Protein C or Protein S deficiencies are associated with severe recurrent thrombotic events. From the clinical standpoint most of the patients are heterozygous, as homozygosity is almost incompatible with life in the absence of a continuous and efficient treatment. Laboratory investigation of this highly complex system involves many different specialized assays for measuring these 3 proteins’ activities, their antigenic content or their genetic sequence. The Protein S in-vitro anticoagulant activity is weak and contrasts with its high antithrombotic role in-vivo, showing that diagnostic assays have not yet succeeded in reproducing all the natural mechanisms for evidencing the anticoagulant role of Protein S. This paradoxal notion is discussed and illustrated in this manuscript as well is a revisit of the major characteristics and pathophysiological functions of the Protein C-Protein S-Thrombomodulin system; the associated pathologies; and the main laboratory tools available for clinical diagnosis. In respect to future perspectives, we also focused on developing more significant and relevant assays, especially for Protein S, thanks to the understanding of its biological roles.

Published

2019

7. A simplified assay for the quantification of circulating activated protein C

Author

Francisco España, Javier Corral, Pilar Medina, E. Bonet, Luis A. Ramón, Laura Martos, Santiago Bonanad, Silvia Navarro, Ana-Rosa Cid, and Manuel Miralles

Subjects

Male, medicine.medical_specialty, Protein C inhibitor, Clinical Biochemistry, 030204 cardiovascular system & hematology, Biochemistry, Gastroenterology, 03 medical and health sciences, 0302 clinical medicine, In vivo, Internal medicine, medicine, Humans, Detection limit, Plasma samples, Chemistry, Biochemistry (medical), Venous Thromboembolism, General Medicine, medicine.disease, Venous thrombosis, Immunology, Conventional PCI, Venous thromboembolism, Protein C, 030215 immunology, medicine.drug

Abstract

Available assays for circulating levels of activated protein C (APC) are either time-consuming or difficult to use in a routine laboratory, or have a detection limit above normal levels. We have developed a simplified assay that measures both the in vivo free APC and the in vivo APC complexed to PC inhibitor (PCI). We measured APC levels, with both assays, in 339 plasma samples, 165 from patients with venous thromboembolism (VTE) and 174 from healthy individuals. The mean APC level in the 339 samples was 0.038±0.010 nM, using a previous assay that measures only the in vivo APC level, and 0.041±0.010 nM with the present new assay. The coefficient of correlation between assays was r=0.954 (P

Published

2016

8. Proteome analysis of testis from infertile protein C inhibitor-deficient mice reveals novel changes in serpin processing and prostaglandin metabolism

Author

Roland Baumgartner, Margarethe Geiger, Pavel Uhrin, Bettina Sarg, Hanjiang Yang, Goran Mitulović, Felix C. Wahlmüller, and Maria Zellner

Subjects

Gel electrophoresis, Molecular mass, Protein C inhibitor, Clinical Biochemistry, Biology, Serpin, Biochemistry, Molecular biology, Analytical Chemistry, Immune system, Downregulation and upregulation, Proteome, Gene

Abstract

Serine protease inhibitors (serpin) have therapeutic potential in a variety of pathogenic processes, ranging from thrombosis and altered immune response to liver cirrhosis. To investigate the physiological effects of protein C inhibitor (PCI, serpinA5), its gene was inactivated in a mouse model, resulting in male infertility. In the present report, 2D differential gel electrophoresis was utilized to investigate the molecular mechanisms for PCI involvement in male reproduction. Comparing the testes proteomes of three PCI-knockout mice with three wild types demonstrated similar patterns with the exception of a massive upregulation of prostaglandin reductase 1 (tenfold; p < 0.002) and the complete shifts in the molecular weights of serpinA1C and serpinA3K. All these PCI-dependent proteome changes were immunologically verified. Unbiased proteome analysis indicated that inactivation of serpinA5 strongly influenced both the protein species pattern of other A-clade serpins as well as prostaglandin metabolism in the testes.

Published

2015

9. Targeting the membrane-anchored serine protease testisin with a novel engineered anthrax toxin prodrug to kill tumor cells and reduce tumor burden

Author

Kathryn H. Driesbaugh, Toni M. Antalis, Stephen H. Leppla, Erik W. Martin, Marguerite S. Buzza, Shihui Liu, and Yolanda M. Fortenberry

Subjects

Proteases, Protein C inhibitor, Anthrax toxin, Bacterial Toxins, Mice, Nude, Antineoplastic Agents, testisin, GPI-Linked Proteins, Protein Engineering, medicine.disease_cause, membrane-anchored serine protease, Serine, Mice, Cell Line, Tumor, medicine, Animals, Humans, Prodrugs, Amino Acid Sequence, Furin, Serine protease, Antigens, Bacterial, biology, Serine Endopeptidases, Proprotein convertase, Xenograft Model Antitumor Assays, Cell biology, HEK293 Cells, Oncology, Biochemistry, biology.protein, anthrax toxin, Female, prodrug, hepsin, Exotoxin, HeLa Cells, Research Paper

Abstract

The membrane-anchored serine proteases are a unique group of trypsin-like serine proteases that are tethered to the cell surface via transmembrane domains or glycosyl-phosphatidylinositol-anchors. Overexpressed in tumors, with pro-tumorigenic properties, they are attractive targets for protease-activated prodrug-like anti-tumor therapies. Here, we sought to engineer anthrax toxin protective antigen (PrAg), which is proteolytically activated on the cell surface by the proprotein convertase furin to instead be activated by tumor cell-expressed membrane-anchored serine proteases to function as a tumoricidal agent. PrAg's native activation sequence was mutated to a sequence derived from protein C inhibitor (PCI) that can be cleaved by membrane-anchored serine proteases, to generate the mutant protein PrAg-PCIS. PrAg-PCIS was resistant to furin cleavage in vitro, yet cytotoxic to multiple human tumor cell lines when combined with FP59, a chimeric anthrax toxin lethal factor-Pseudomonas exotoxin fusion protein. Molecular analyses showed that PrAg-PCIS can be cleaved in vitro by several serine proteases including the membrane-anchored serine protease testisin, and mediates increased killing of testisin-expressing tumor cells. Treatment with PrAg-PCIS also potently attenuated the growth of testisin-expressing xenograft tumors in mice. The data indicates PrAg can be engineered to target tumor cell-expressed membrane-anchored serine proteases to function as a potent tumoricidal agent.

Published

2015

10. 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

11. Safety and Antithrombotic Efficacy of the Recombinant Protein C Activator AB002 (E-WE Thrombin) in End Stage Renal Disease Patients on Chronic Hemodialysis

Author

Norah G. Verbout, Erik I. Tucker, Christina U. Lorentz, Andras Gruber, Joseph J. Shatzel, and Brandon D. Markway

Subjects

Activator (genetics), business.industry, Protein C inhibitor, medicine.medical_treatment, Immunology, Cell Biology, Hematology, Pharmacology, Thrombomodulin, Biochemistry, End stage renal disease, Thrombin, Antithrombotic, medicine, Hemodialysis, business, Fibrinolytic agent, medicine.drug

Abstract

AB002 is a recombinant thrombin analog that generates endogenous activated protein C (APC) on intravascular surfaces in a thrombomodulin-dependent manner but does not promote thrombosis. Endogenously generated APC downregulates thrombin generation, thereby reducing pathological clot formation. During hemodialysis (HD), thrombi can form within the dialyzer filter and circuit, reducing dialyzer efficiency, and increasing blood loss. Heparin administration reduces clotting within the filter and circuit, but increases bleeding risk and is not tolerated in all patients. Since end-stage renal disease (ESRD) patients undergoing HD are at higher risk of both thromboembolism and bleeding, a safe, short-term and self-limiting anticoagulant alternative to heparin is currently an unmet need for this population. This is a phase 2, randomized, double-blind, placebo-controlled, single-dose study designed to evaluate the safety and efficacy of AB002 at two dose levels when administered to ESRD patients during heparin-free HD. A total of 36 adult patients are planned to be enrolled into two cohorts and dosed sequentially. Within each cohort, patients will be randomized to active drug (12) or placebo (6). Dose levels (1.5 µg/kg or 3 µg/kg; iv infusion) were based on safety data from a completed phase 1 study performed in healthy adult subjects (NCT03453060), which demonstrated that a single dose of AB002 was well tolerated, as well as based on preclinical efficacy studies performed in a baboon vascular thrombosis model. The primary objective of this phase 2 proof-of-concept study is safety and tolerability assessed as the number and severity of adverse events (AE), changes in baseline physical and lab parameters and immunogenicity of AB002. The number and severity of AE will be tabulated and summary statistics evaluated. The secondary objectives are to assess 1) pharmacodynamics using activated protein C/protein C inhibitor complexes in plasma as a surrogate marker for drug exposure, and 2) efficacy via pre-post dialyzer pressures, visual inspection of thrombus accumulation in the HD filter and dialysis efficiency based on urea kinetics. The study population includes ESRD patients on a stable outpatient HD regimen at least 3 times per week and excludes patients with history of acute vaso-occlusive thrombotic events, concomitant use of anticoagulant/antiplatelet agents immediately prior to and during the study, active cancer and bleeding disorders. This study is currently recruiting participants at one study site (Orlando Clinical Research Center) in Orlando, FL and is estimated to complete in October 2020 (NCT03963895). Disclosures Verbout: Aronora, Inc.: Employment, Equity Ownership. Lorentz:Aronora, Inc.: Employment. Markway:Aronora, Inc.: Employment. Shatzel:Aronora, Inc.: Consultancy. Tucker:Aronora, Inc.: Employment, Equity Ownership. Gruber:Aronora, Inc.: Employment, Equity Ownership.

Published

2019

12. Cell penetrating SERPINA5 (ProteinC inhibitor, PCI): More questions than answers

Author

Margarethe Geiger and Hanjiang Yang

Subjects

0301 basic medicine, media_common.quotation_subject, Protein C inhibitor, Cell, Retinoic acid, Serpin, Biology, Ligands, 03 medical and health sciences, chemistry.chemical_compound, medicine, Animals, Humans, Internalization, media_common, Protein C Inhibitor, Urokinase, Cell Nucleus, Cell Biology, Endocytosis, Protein Transport, 030104 developmental biology, medicine.anatomical_structure, chemistry, Biochemistry, Models, Animal, Plasminogen activator, Intracellular, Developmental Biology, medicine.drug

Abstract

SERPINA5 (proteinC inhibitor, plasminogen activator inhibitor-3) is a secreted, extracellular clade A serpin. Its main characteristics are broad protease reactivity and wide tissue distribution (in man). SERPINA5 has originally been described as an inhibitor of activated protein C and independently as an inhibitor of the plasminogen activator urokinase. SERPINA5 binds glycosaminoglycans, phospholipids, and retinoic acid. Glycosaminoglycans and certain phospholipids can modulate its inhibitory activity and specificity. Studies suggest that SERPINA5 may play a role in hemostasis, in male reproduction, in host defense, and as a tumor suppressor. However, its biological role has not yet been defined. So far SERPINA5 deficiency has not been described in man. Mouse models are of limited value, since in mice serpinA5 is almost exclusively expressed in the reproductive tract. Consistently the only obvious phenotype of serpinA5-knockout mice is infertility of homozygous males. SERPINA5 can be internalized by cells and translocated to the nucleus. The internalization is dependent on the phospholipid phosphatidylethanolamine and on the intact N-terminus of SERPINA5, which functions as a cell penetrating peptide. Further functional analysis of intracellular SERPINA5 will contribute to our understanding of the biological role of this molecule.

Published

2016

13. Role of heparin and non heparin binding serpins in coagulation and angiogenesis: A complex interplay

Author

Mohammad Farhan Ali, Shadabi Bano, Mohamad Aman Jairajpuri, Teena Bhakuni, Irshad Ahmad, and S. G. Ansari

Subjects

0301 basic medicine, Angiogenesis, Cell, Biophysics, Angiotensinogen, Molecular Conformation, Inflammation, Biology, Biochemistry, Antithrombins, Extracellular matrix, 03 medical and health sciences, Plasminogen Activator Inhibitor 1, Serpin E2, medicine, Animals, Homeostasis, Humans, Nerve Growth Factors, Eye Proteins, Molecular Biology, Blood Coagulation, Serpins, Protein C Inhibitor, Neovascularization, Pathologic, Heparin, Fibrinolysis, Anticoagulants, Blood Proteins, Heparin, Low-Molecular-Weight, medicine.disease, Thrombosis, Extracellular Matrix, carbohydrates (lipids), 030104 developmental biology, medicine.anatomical_structure, Coagulation, Hemostasis, Immunology, Cancer research, Disease Progression, Blood Vessels, medicine.symptom, Heparan Sulfate Proteoglycans, medicine.drug, Signal Transduction

Abstract

Pro-coagulant, anti-coagulant and fibrinolytic pathways are responsible for maintaining hemostatic balance under physiological conditions. Any deviation from these pathways would result in hypercoagulability leading to life threatening diseases like myocardial infarction, stroke, portal vein thrombosis, deep vein thrombosis (DVT) and pulmonary embolism (PE). Angiogenesis is the process of sprouting of new blood vessels from pre-existing ones and plays a critical role in vascular repair, diabetic retinopathy, chronic inflammation and cancer progression. Serpins; a superfamily of protease inhibitors, play a key role in regulating both angiogenesis and coagulation. They are characterized by the presence of highly conserved secondary structure comprising of 3 β-sheets and 7-9 α-helices. Inhibitory role of serpins is modulated by binding to cofactors, specially heparin and heparan sulfate proteoglycans (HSPGs) present on cell surfaces and extracellular matrix. Heparin and HSPGs are the mainstay of anti-coagulant therapy and also have therapeutic potential as anti-angiogenic inhibitors. Many of the heparin binding serpins that regulate coagulation cascade are also potent inhibitors of angiogenesis. Understanding the molecular mechanism of the switch between their specific anti-coagulant and anti-angiogenic role during inflammation, stress and regular hemostasis is important. In this review, we have tried to integrate the role of different serpins, their interaction with cofactors and their interplay in regulating coagulation and angiogenesis.

Published

2016

14. 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

15. Structural biology of the PCI-protein fold

Author

Andrew M. Ellisdon and Murray Stewart

Subjects

Models, Molecular, Proteasome Endopeptidase Complex, Protein Folding, Saccharomyces cerevisiae Proteins, Protein C inhibitor, Mini Review, Biology, TREX-2 complex, Protein Structure, Secondary, COP9 complex, Structural Biology, PCI protein, Nucleic Acids, Humans, COP9 signalosome, Protein C Inhibitor, PCI fold, Cell Biology, General Medicine, Fold (geology), Elongation factor, proteasome, Proteasome, Structural biology, Biochemistry, Biophysics, Nucleic acid, Protein folding, eIF3

Abstract

The PCI fold is based on a stack of α-helices topped with a winged-helix domain and is found in a range of proteins that form central parts of large complexes such as the proteasome lid, the COP9 signalosome, elongation factor eIF3, and the TREX-2 complex. Recent structural determinations have given intriguing insight into how these folds function both to facilitate the generation of larger proteinaceous assembles and also to interact functionally with nucleic acids.

Published

2012

16. A Novel Heparin-dependent Inhibitor of Activated Protein C That Potentiates Consumptive Coagulopathy in Russell's Viper Envenomation

Author

Guey Yueh Shi, An-Chun Cheng, Inn Ho Tsai, and Hua Lin Wu

Subjects

DNA, Complementary, Molecular Sequence Data, Viper Venoms, Biology, Fibrinogen, Biochemistry, Fibrin, Mice, Consumptive Coagulopathy, medicine, Animals, Humans, Russell's Viper, Amino Acid Sequence, Cloning, Molecular, Blood Coagulation, Molecular Biology, Protein C Inhibitor, Serine protease, Mice, Inbred ICR, Sequence Homology, Amino Acid, Heparin, Drug Synergism, Sequence Analysis, DNA, Cell Biology, Disseminated Intravascular Coagulation, Molecular biology, Kinetics, Coagulation, Snake venom, Enzymology, biology.protein, Carrier Proteins, Protein C, Protein Binding, medicine.drug

Abstract

The activation of coagulation factors V and X by Russell's viper venom (RVV) has been implicated in the development of consumptive coagulopathies in severely envenomed patients. However, factor Va is prone to inactivation by activated protein C (APC), an important serine protease that negatively regulates blood coagulation. It is therefore hypothesized that APC may be down-regulated by some of the venom components. In this study, we managed to isolate a potent Kunitz-type APC inhibitor, named DrKIn-I. Using chromogenic substrate, DrKIn-I dose-dependently inhibited the activity of APC. Heparin potentiated the inhibition and reduced the IC(50) of DrKIn-I by 25-fold. DrKIn-I, together with heparin, also protected factor Va from APC-mediated inactivation. Using surface plasmon resonance, DrKIn-I exhibited fast binding kinetics with APC (association rate constant = 1.7 × 10(7) M(-1) s(-1)). Direct binding assays and kinetic studies revealed that this inhibition (K(i) = 53 pM) is due to the tight binding interactions of DrKIn-I with both heparin and APC. DrKIn-I also effectively reversed the anticoagulant activity of APC and completely restored the thrombin generation in APC-containing plasma. Furthermore, although the injection of either DrKIn-I or RVV-X (the venom factor X-activator) into ICR mice did not significantly deplete the plasma fibrinogen concentration, co-administration of DrKIn-I with RVV-X resulted in complete fibrinogen consumption and the deposition of fibrin thrombi in the glomerular capillaries. Our results provide new insights into the pathogenesis of RVV-induced coagulopathies and indicate that DrKIn-I is a novel APC inhibitor that is associated with potentially fatal thrombotic complications in Russell's viper envenomation.

Published

2012

17. Toxicological biomarkers of 2,3,4,7,8-pentachlorodibenzofuran in proteins secreted by HepG2 cells

Author

Zhi Zheng, Eunkyung Cho, Nam Hee Won, Woon Won Jung, Sohee Phark, So Young Park, Ji Youn Lim, Min Lee, Jong Bok Seo, Seonyoung Choi, and Donggeun Sul

Subjects

Male, Proteomics, Proteasome Endopeptidase Complex, Spectrometry, Mass, Electrospray Ionization, Proteome, Cell Survival, Protein subunit, Protein Deglycase DJ-1, Biophysics, Biochemistry, Analytical Chemistry, Rats, Sprague-Dawley, Western blot, medicine, Animals, Humans, Electrophoresis, Gel, Two-Dimensional, MTT assay, Proteasome activator complex, education, Molecular Biology, Benzofurans, Cell Proliferation, Protein C Inhibitor, Oncogene Proteins, education.field_of_study, Two-dimensional gel electrophoresis, medicine.diagnostic_test, Chemistry, Intracellular Signaling Peptides and Proteins, Hep G2 Cells, Molecular biology, Blood proteins, Rats, Up-Regulation, Environmental Pollutants, Comet Assay, Plasminogen activator, Biomarkers, DNA Damage, Nucleoside diphosphate kinase A

Abstract

Using a proteomic approach, a study was conducted for determination of the effects of 2,3,4,7,8-pentachlorodibenzofuran (2,3,4,7,8-PCDF) on proteins secreted by HepG2 cells. Briefly, HepG2 cells were exposed to various concentrations of 2,3,4,7,8-PCDF for 24 or 48 h. MTT and comet assays were then conducted for determination of cytotoxicity and genotoxicity, respectively. Results of an MTT assay showed that 1 nM of 2,3,4,7,8-PCDF was the maximum concentration that did not cause cell death. In addition, a dose- and time dependent increase of DNA damage was observed in HepG2 cells exposed to 2,3,4,7,8-PCDF. Therefore, two different concentrations of 2,3,4,7,8-PCDF, 1 and 5 nM, were selected for further analysis of proteomic biomarkers using two different pI ranges (4–7 and 6–9) and large two dimensional gel electrophoresis. Results showed identification of 32 proteins ( 29 up- and 3 down-regulated) by nano-LC-ESI-MS/MS and nano-ESI on a Q-TOF2 MS. Among these, the identities of pyridoxine-5'-phosphate oxidase, UDP-glucose 6-dehydrogenase, plasminogen activator inhibitor I precursor, plasminogen activator inhibitor-3, proteasome activator complex subunit 1, isoform 1 of 14-3-3 protein sigma, peptidyl-prolyl cis-trans isomerase A, 14-3-3 protein gamma, protein DJ-1, and nucleoside diphosphate kinase A were confirmed by western blot analysis. The differential expression of protein DJ-1, proteasome activator complex subunit 1 and plasminogen activator inhibitor-3 was further validated in plasma proteins from rats exposed to 2,3,4,7,8-PCDF. These proteins could be used as potential toxicological biomarkers of 2,3,4,7,8-PCDF.

Published

2012

18. Precision of Heavy–Light Peptide Ratios Measured by MALDI-TOF Mass Spectrometry

Author

Rainer Paape, N. Leigh Anderson, Gary Kruppa, Morteza Razavi, Terry W. Pearson, and Detlef Suckau

Subjects

Proteomics, Molecular Sequence Data, Analytical chemistry, Peptide, Mass spectrometry, Biochemistry, Humans, Trypsin, Amino Acid Sequence, Peptide sequence, Protein C Inhibitor, chemistry.chemical_classification, Peak area, Chromatography, Spots, Chemistry, Stable isotope ratio, General Chemistry, Reference Standards, MALDI-TOF Mass Spectrometry, Peptide Fragments, Dilution, Molecular Weight, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, Calibration, Proteolysis

Abstract

We have investigated the precision of peptide quantitation by MALDI-TOF mass spectrometry (MS) using six pairs of proteotypic peptides (light) and same-sequence stable isotope labeled synthetic internal standards (heavy). These were combined in two types of dilution curves spanning 100-fold and 2000-fold ratios. Coefficients of variation (CV; standard deviation divided by mean value) were examined across replicate MALDI spots using a reflector acquisition method requiring 100 000 counts for the most intense peak in each summed spectrum. The CV of light/heavy peptide centroid peak area ratios determined on four replicate spots per sample, averaged across 11 points of a 100-fold dilution curve and over all six peptides, was 2.2% (ranging from 1.5 to 3.7% among peptides) at 55 fmol total (light + heavy) of each peptide applied per spot, and 2.5% at 11 fmol applied. The average CV of measurements at near-equivalence (light = heavy, the center of the dilution curve) for the six peptides was 1.0%, about 17-fold lower CV than that observed when five peptides were ratioed to a sixth peptide (i.e., a different-sequence internal standard). Response curves across the 100-fold range were not completely linear but could be closely modeled by a power law fit giving R(2) values0.998 for all peptides. The MALDI-TOF MS method was used to determine the endogenous level of a proteotypic peptide (EDQYHYLLDR) of human protein C inhibitor (PCI) in a plasma digest after enrichment by capture on a high affinity antipeptide antibody, a technique called stable isotope standards and capture by anti-peptide antibodies (SISCAPA). The level of PCI was determined to be 770 ng/mL with a replicate measurement CV of 1.5% and a14 000-fold target enrichment via SISCAPA-MALDI-TOF. These results indicate that MALDI-TOF technology can provide precise quantitation of high-to-medium abundance peptide biomarkers over a 100-fold dynamic range when ratioed to same-sequence labeled internal standards and enriched to near purity by specific antibody capture. The robustness and throughput of MALDI-TOF in comparison to conventional nano-LC-MS technology could enable currently impractical large-scale verification studies of protein biomarkers.

Published

2012

19. Antibodies associated with heparin-induced thrombocytopenia (HIT) inhibit activated protein C generation: new insights into the prothrombotic nature of HIT

Author

Sriram Krishnaswamy, Karine Amirikian, Lubica Rauova, Douglas B. Cines, Vincent Hayes, Richard H. Aster, Jeffrey D. Esko, Mortimer Poncz, Daniel W. Bougie, M. Anna Kowalska, and Li Zhai

Subjects

Adult, Protamine sulfate, Thrombomodulin, Protein C inhibitor, Immunology, Kidney, Platelet Factor 4, Biochemistry, Thrombosis and Hemostasis, Mice, chemistry.chemical_compound, Thrombin, Heparin-induced thrombocytopenia, medicine, Animals, Humans, Chondroitin sulfate, Cells, Cultured, Glycosaminoglycans, Protein C Inhibitor, Mice, Knockout, Integrases, Heparin, Antibodies, Monoclonal, Anticoagulants, Kidney metabolism, Cell Biology, Hematology, medicine.disease, Thrombocytopenia, Molecular biology, Recombinant Proteins, Mice, Inbred C57BL, chemistry, Prothrombin, Protein Multimerization, Platelet factor 4, Protein C, medicine.drug

Abstract

Heparin-induced thrombocytopenia (HIT) is caused by antibodies that recognize complexes between platelet factor 4 (PF4) and heparin or glycosaminoglycan side chains. These antibodies can lead to a limb- and life-threatening prothrombotic state. We now show that HIT antibodies are able to inhibit generation of activated protein C (aPC) by thrombin/thrombomodulin (IIa/TM) in the presence of PF4. Tetrameric PF4 potentiates aPC generation by formation of complexes with chondroitin sulfate (CS) on TM. Formation of these complexes occurs at a specific molar ratio of PF4 to glycosaminoglycan. This observation and the finding that the effect of heparin on aPC generation depends on the concentration of PF4 suggest similarity between PF4/CS complexes and those that bind HIT antibodies. HIT antibodies reduced the ability of PF4 to augment aPC formation. Cationic protamine sulfate, which forms similar complexes with heparin, also enhanced aPC generation, but its activity was not blocked by HIT antibodies. Our studies provide evidence that complexes formed between PF4 and TM's CS may play a physiologic role in potentiating aPC generation. Recognition of these complexes by HIT antibodies reverses the PF4-dependent enhancement in aPC generation and may contribute to the prothrombotic nature of HIT.

Published

2011

20. Recent advances in the development of coagulation factors and procoagulants for the treatment of hemophilia

Author

Robert G. Schaub

Subjects

Excessive Bleeding, Lipoproteins, Factor VIIa, Hemophilia A, Biochemistry, law.invention, Factor IX, law, hemic and lymphatic diseases, medicine, Coagulopathy, Animals, Humans, In patient, Protein C Inhibitor, Pharmacology, Factor VIII, business.industry, medicine.disease, Blood Coagulation Factors, Recombinant Proteins, Antibody response, Coagulation, Factor Xa, Immunology, Recombinant DNA, Normal blood, business, medicine.drug

Abstract

Hemophilia is a family of rare bleeding disorders. The two primary types, hemophilia A and hemophilia B, are caused by recessive X-chromosome linked mutations that result in deficiency of coagulation factor VIII (FVIII) or factor IX (FIX), respectively. Clinically, hemophilia is manifested by spontaneous bleeding, particularly into the joints (haemarthrosis) and soft tissue, and excessive bleeding following trauma or surgery. The total overall number of hemophilia patients worldwide is approximately 400,000, however only about 100,000 of these individuals are treated. The first treatment of hemophilia was initiated when it was determined that the clotting deficiency could be corrected by a plasma fraction taken from normal blood. The discovery of factor VIII enrichment by cryoprecipitation of plasma opened a new era of therapy which eventually led to the production of factor concentrates and the subsequent development of highly purified forms of plasma factors. The most significant improvements have been the availability of recombinant forms of factors VIII and IX. Unfortunately, recombinant factors still retain some of the limitations of plasma concentrates. These limitations include development of antibody responses in patients and the relatively short half-life of the molecules requiring frequent injection to maintain effective concentration. Treatment beyond replacement of native factors has been tried. They include the development of modified factor VIII and IX molecules with improved potency, stability and circulating half-life and enhancement of a prothrombotic responses and/or stabilization of coagulation factors via inhibition of key negative regulatory pathways. These approaches will be reviewed in this commentary.

Published

2011

21. Protein C Inhibitor

Author

Heiko Herwald, Joost C. M. Meijers, Amsterdam Cardiovascular Sciences, and Vascular Medicine

Subjects

Serine protease, Hemostasis, Proteases, biology, Fibrinolysis, medicine.medical_treatment, Protein C inhibitor, Thrombosis, Hematology, Serpin, surgical procedures, operative, Coagulation, Biochemistry, Conventional PCI, medicine, biology.protein, Animals, Humans, cardiovascular diseases, Cardiology and Cardiovascular Medicine, Protein C, Protein C Inhibitor, medicine.drug

Abstract

Protein C inhibitor (PCI) is a serine protease inhibitor and was originally identified as an inhibitor of activated protein C (APC). However, PCI is not specific for APC and also inhibits several proteases involved in coagulation, fibrinolysis, cancer, wound healing, and fertility. The biological function of PCI is unknown due to broad enzyme specificity, its wide tissue distribution, and the lack of a suitable animal model. This review highlights the specific roles of PCI in the areas of hemostasis and thrombosis and fertilization, and it also describes the latest information on the fascinating participation of the protein in intracellular processes, phospholipid binding, and killing of bacteria.

Published

2011

22. A Direct Oral Anticoagulant Edoxaban Enhanced Fibrinolysis Via Inhibition of Thrombin-Activatable Fibrinolysis Inhibitor Activation and Enhancement of Plasmin Generation in Human Plasma

Author

Yoshiyuki Morishima, Yuko Honda, and Taketoshi Furugohri

Subjects

medicine.drug_mechanism_of_action, Plasmin, Protein C inhibitor, medicine.medical_treatment, Immunology, Factor Xa Inhibitor, Cell Biology, Hematology, Pharmacology, Thrombomodulin, Biochemistry, chemistry.chemical_compound, chemistry, Edoxaban, Alpha 2-antiplasmin, Fibrinolysis, medicine, Thromboplastin, medicine.drug

Abstract

Introduction: Direct oral anticoagulants are as effective as vitamin K antagonists for the treatment of venous thromboembolism and are associated with less bleeding. We have reported that a direct oral factor Xa inhibitor edoxaban exerts a thrombus resolution effect in a rat model of venous thrombosis and enhances tissue plasminogen activator (t-PA)-induced clot lysis in human plasma. However, the mechanism underlying the thrombus resolution effect and fibrinolysis enhancement by edoxaban remains to be determined. Purposes: To evaluate the effect of edoxaban on plasmin generation during clot lysis in human plasma in vitro. To determine the role of thrombin-activatable fibrinolysis inhibitor (TAFI) in the enhancement of fibrinolysis by edoxaban. Methods: Pooled human normal plasma or TAFI-deficient plasma (both containing 180 ng/mL t-PA and 0.1 nM thrombomodulin) was mixed with edoxaban, an activated TAFI (TAFIa) inhibitor (a fibrinolysis enhancer) potato tuber carboxypeptidase inhibitor (PCI), or vehicle. Clot was induced by adding 2.5 pM tissue factor and 4 µM phospholipids. To monitor the clot formation and lysis, the absorbance of plasma at 405 nm was measured every 30 sec. Clot lysis time was defined as the interval between the time of the midpoint of the clear to maximum turbidity transition and the midpoint of the maximum turbidity to clear transition. Plasmin-α2 antiplasmin complex (PAP) concentration was measured by ELISA as an indicator of plasmin generation. Results: In normal plasma, PCI accelerated clot lysis and increased plasma PAP concentration. There was a correlation between plasma PAP concentration and percent of clot lysis, indicating that plasma PAP concentration is an appropriate marker of fibrinolysis. Edoxaban at clinically relevant concentrations (75, 150, and 300 ng/mL) significantly shortened clot lysis time and elevated plasma PAP concentration. The additive combined effect of edoxaban and PCI was observed. In TAFI-deficient plasma, clot lysis time was shortened and plasma PAP concentration increased compared with normal plasma. In these samples, the effects of edoxaban and PCI on clot lysis and plasma PAP concentration were markedly diminished as compared with normal plasma. Conclusions: Edoxaban at clinically relevant concentrations enhanced t-PA-induced clot lysis with increasing plasma PAP concentration in human plasma. The effects of edoxaban on clot lysis and plasmin generation were diminished in TAFI-deficient plasma. A TAFIa inhibitor PCI exerted similar effects. These data suggest that edoxaban enhanced fibrinolysis via inhibition of TAFI activation and enhancement of plasmin generation. Disclosures Morishima: Daiichi Sankyo Co., Ltd.: Employment. Honda:Daiichi Sankyo Co., Ltd.: Employment. Furugohri:Daiichi Sankyo Co., Ltd.: Employment.

Published

2018

23. Efficacy of Anti-TFPI Antibody PF-06741086 Alone and in Combination with Activated Prothrombin Complex Concentrates in Mouse Hemophilia a Bleeding Model

Author

Amey Barakat, Reema Jasuja, John E. Murphy, and Debra D. Pittman

Subjects

biology, business.industry, Protein C inhibitor, Immunology, Cell Biology, Hematology, Pharmacology, medicine.disease, Biochemistry, Hemostatics, Bleeding diathesis, Tissue factor pathway inhibitor, Anti-Inhibitor Coagulant Complex, medicine, biology.protein, Thromboplastin, Antibody, business, Factor IX, medicine.drug

Abstract

BACKGROUND: Tissue Factor Pathway inhibitor (TFPI) is a plasma serine protease inhibitor that modulates the initiation of coagulation by directly binding and inhibiting the Tissue Factor (TF)/Factor VIIa/Factor Xa complex. TFPI is a multi-Kunitz domain protein that directly binds to and inhibits both activated Factor Xa (FXa) and FVIIa. Blocking TFPI can act as a bypass therapy by facilitating hemostasis initiated by tissue factor/FVIIa, thereby, compensating for loss of Factor VIII or Factor IX (in hemophilia A or B). PF-06741086, a fully human antibody engineered to inhibit TFPI, exhibits broad cross reactivity to TFPI from numerous species, including mouse. PF-06741086 is being developed as a potential treatment for bleeding disorders including hemophilia A and hemophilia B with and without inhibitors. aPCC (activated Prothrombin complex concentrates or FEIBA, Factor Eight Inhibitor Bypass Agent) is a bypass agent for to control bleed in Hemophilia patients with inhibitors. Since it is a plasma-derived concentrate containing various prothrombin complex coagulation factors in their enzymatic or zymogen form, it is possible that FEIBA could potentially impact the activity of PF-06741086. AIMS: Here, we directly compare the hemostatic effect of PF-06741086 alone, and in combination with aPCC in Hemophilia A mouse model using severe tail vein transection. METHODS: Male hemophilia A mice were dosed with a single intravenous dose of PF-06741086 (0.5, 1, 2 or 6 mg/kg) 30 minutes prior to a 3mm tail clip, or aPCC (50, 100 or 200 U/kg) was administered 5 minutes before the tail clip. Mice were also treated with a combined dose of 0.5 mg/kg anti-TFPI PF-06741086 and aPCC at 50, 100 or 200 U/kg. Blood was collected for 10 minutes and quantified against a standard curve of hemoglobin as volume blood loss. RESULTS: PF-06741086 demonstrated a dose dependent response in improving hemostasis in Hemophilia A mice after tail clip. PF-06741086 was able to restore hemostasis at 1 mg/kg (49%), and higher doses further improved hemostasis at 2 mg/kg (63%), and 6 mg/kg (78%). aPCC also demonstrated a dose dependent reduction in blood loss and improved hemostasis with all tested doses of 50 U/kg (25%), 100 U/kg (23%) and 200 U/kg (66%). At a dose of 0.5 mg/kg, PF-06741086 did not show any improvement in hemostasis over vehicle control. We used this dose for all combination studies with aPCC. Combined use of low dose PF-06741086 (0.5 mg/kg) and 100 U/kg aPCC shows a trend towards improvement in hemostasis compared to either drug alone. A higher dose of aPCC (200 U/kg) combined with low dose PF-06741086 (0.5 mg/kg) significantly reduces blood loss (86%) in Hemophilia A mice in tail clip model compared to saline, TFPI or aPCC alone used at the same dose of 0.5 mg/kg or 200 U/kg respectively. CONCLUSIONS: Prophylactic administration of PF-06741086 exhibits a dose response and improves hemostasis in an injury model in Hemophilia A mice. The addition of aPCC alone restores hemostasis at 200 U/kg and this effect was enhanced in combination with PF-06741086 in this mouse model. Disclosures Barakat: Pfizer: Employment. Jasuja:Pfizer: Employment. Murphy:Pfizer: Employment. Pittman:Pfizer: Employment.

Published

2018

24. Protein C inhibitor regulates both cathepsin L activity and cell-mediated tumor cell migration

Author

Yolanda M. Fortenberry, Stephanie Brandal, Frank C. Church, and Ryan C. Bialas

Subjects

Cathepsin L, Protein C inhibitor, Biophysics, Fluorescent Antibody Technique, Cathepsin D, Breast Neoplasms, Serpin, Biochemistry, Plasma Serine Protease Inhibitor, Cell Line, Tumor, Cathepsin L1, Humans, cardiovascular diseases, Neoplasm Metastasis, Molecular Biology, DNA Primers, Protein C Inhibitor, Cathepsin S, Cathepsin, Base Sequence, biology, Molecular biology, surgical procedures, operative, Mutagenesis, Site-Directed, biology.protein

Abstract

Background Protein C inhibitor (PCI) is a plasma serine protease inhibitor (serpin) that regulates several serine proteases in coagulation including thrombin and activated protein C. However, the physiological role of PCI remains under investigation. The cysteine protease, cathepsin L, has a role in many physiological processes including cardiovascular diseases, blood vessel remodeling, and cancer. Methods and results We found that PCI inhibits cathepsin L with an inhibition rate (k 2 ) of 3.0 × 10 5 M − 1 s − 1 . Whereas, the PCI P1 mutant (R354A) inhibits cathepsin L at rates similar to wild-type PCI, mutating the P2 residue results in a slight decrease in the rate of inhibition. We then assessed the effect of PCI and cathepsin L on the migration of human breast cancer (MDA-MB-231) cells. Cathepsin L was expressed in both the cell lysates and conditioned media of MDA-MB-231 cells. Wound-induced and transwell migration of MDA-MB-231 cells was inhibited by exogenously administered wtPCI and PCI P1 but not PCI P14 mutant. In addition, migration of MDA-MB-231 cells expressing wtPCI was significantly decreased compared to non-expressing MDA-MB-231 cells or MDA-MB-231 cells expressing the PCI P14 mutant. Downregulation of cathepsin L by either a specific cathepsin L inhibitor or siRNA technology also resulted in a decrease in the migration of MDA-MB-231 cells. Conclusions Overall, our data show that PCI regulates tumor cell migration partly by inhibiting cathepsin L. General significance Consequently, inhibiting cathepsin L by serpins like PCI may be a new pathway of regulating hemostasis, cardiovascular and metastatic diseases.

Published

2010

25. Hepatocyte growth factor activator (HGFA): its regulation by protein C inhibitor

Author

Koji Suzuki

Subjects

Serine protease, biology, Protein C inhibitor, Cell Biology, Hepatocyte Growth Factor Activator, Biochemistry, Liver regeneration, Plasma Serine Protease Inhibitor, surgical procedures, operative, biology.protein, medicine, Hepatic stellate cell, Cancer research, Hepatocyte growth factor, cardiovascular diseases, Molecular Biology, Protein C, medicine.drug

Abstract

Protein C inhibitor (PCI; SERPINA5) is a plasma serine protease inhibitor, and a potent inhibitor of activated protein C (APC), which plays a critical role in the anticoagulant protein C pathway. Recently, PCI was also found to form a complex with the serine protease hepatocyte growth factor activator (HGFA), inhibiting the HGFA-catalyzed activation of the single-chain hepatocyte growth factor precursor. In vivo studies using human PCI-transgenic (hPCI-Tg) mice, which mimic PCI expression in humans, showed that the regeneration rate of the liver after partial hepatectomy was significantly impaired as compared with wild-type mice. The decreased liver regeneration in hPCI-Tg mice was restored by pretreatment with antibody against human PCI. Furthermore, APC protected hepatic nonparenchymal cells from thrombin-induced inflammation in vitro, suggesting that plasma PCI may inhibit the cytoprotective action of APC on hepatic cells in hPCI-Tg mice. It was shown that the levels of HGFA-PCI are increased in plasma of patients who have been subjected to hepatectomy, as compared with complex levels in the plasma of normal individuals. Thus, PCI may play a role as a potent inhibitor of HGFA and APC in plasma and/or at the sites of tissue injury in the regulation of tissue regeneration.

Published

2010

26. Cytokines and systemic biomarkers are related to the size of abdominal aortic aneurysms

Author

Anders Gottsäter, Despina Flondell-Sité, Tilo Kölbel, and Bengt Lindblad

Subjects

medicine.medical_specialty, Pathology, Statistics as Topic, Immunology, Inflammation, Biochemistry, Gastroenterology, Aortic aneurysm, chemistry.chemical_compound, Aneurysm, Internal medicine, medicine, Humans, Immunology and Allergy, Prospective Studies, cardiovascular diseases, Prospective cohort study, Molecular Biology, Aged, Protein C Inhibitor, Aged, 80 and over, Creatinine, Interleukin-6, business.industry, Interleukin, Hematology, Middle Aged, medicine.disease, Abdominal aortic aneurysm, chemistry, cardiovascular system, Cytokines, Female, medicine.symptom, Endothelin receptor, business, Biomarkers, Aortic Aneurysm, Abdominal

Abstract

Objective: The etiology of abdominal aortic aneurysm (AAA) includes atherosclerotic, inflammatory, immunological and coagulatory mechanisms. The aim of this study was to evaluate associations between markers for some of these mechanisms and AAA-size, in order to identify markers which might later be evaluated in relation to aneurysm growth. Material and methods: Prospectively 360 AAA-patients and an age and sex-matched healthy control group (n=219) were analyzed. AAA-patients were divided in three groups according to AAA-diameter (small 55mm, n=130). Associated diseases, blood pressures and routine laboratory markers were analyzed. Additionally we evaluated endothelin (ET)-1, tumour necrosis factor (TNF)-alpha, interleukin (IL)-6, activated protein C-protein C inhibitor (APC-PCI) complex, and CD40 ligand. Groups were compared with the Kruskall-Wallis test and the Mann-Whitney U test. Results: Of routine markers platelet count was lower (p=0.0006) and creatinine level was higher (p=0.028) in patients with large AAA. Almost all non-routine markers analyzed were highly elevated in AAA-patients compared to the control group. IL-6 (p=0.0002) and thrombin activation measured as APC-PCI (p

Published

2009

27. An Exosite-Specific ssDNA Aptamer Inhibits the Anticoagulant Functions of Activated Protein C and Enhances Inhibition by Protein C Inhibitor

Author

Mohammad Salehi, Bernd Pötzsch, Jens Müller, Johannes Oldenburg, Günter Mayer, Max J. Friedrich, Berend Isermann, Thati Madhusudhan, Christina Dücker, and Moritz Meyer

Subjects

medicine.drug_class, Protein C inhibitor, medicine.medical_treatment, Aptamer, Clinical Biochemistry, Apoptosis, Biochemistry, law.invention, law, Drug Discovery, medicine, Humans, Binding site, Enzyme Inhibitors, Molecular Biology, Serine protease, Pharmacology, Protease, biology, Chemistry, Anticoagulant, SELEX Aptamer Technique, Thrombin, Anticoagulants, General Medicine, DNA, Aptamers, Nucleotide, CHEMBIO, Recombinant DNA, biology.protein, Molecular Medicine, Protein C, medicine.drug, Protein Binding

Abstract

SummaryActivated protein C (APC) is a serine protease with anticoagulant, anti-inflammatory, and cytoprotective properties. Using recombinant APC, we identified a class of single-stranded DNA aptamers (HS02) that selectively bind to APC with high affinity. Interaction of HS02 with APC modulates the protease activity in a way such that the anticoagulant functions of APC are inhibited and its reactivity toward the protein C inhibitor is augmented in a glysoaminoglycan-like fashion, whereas APC's antiapoptotic and cytoprotective functions remain unaffected. Based on these data, the binding site of HS02 was localized to the basic exosite of APC. These characteristics render the exosite-specific aptamers a promising tool for the development of APC assays and a potential therapeutic agent applicable for the selective control of APC's anticoagulant activity.

Published

2009

28. N-Glycans and the N Terminus of Protein C Inhibitor Affect the Cofactor-enhanced Rates of Thrombin Inhibition

Author

Anne Dell, Howard R. Morris, Wei Sun, Maria Panico, Simon Parry, Åke Engström, Margareta Kjellberg, and Sophia Schedin-Weiss

Subjects

Glycan, Proteases, Glycosylation, Thrombomodulin, medicine.medical_treatment, Protein C inhibitor, Biochemistry, Fucose, Substrate Specificity, chemistry.chemical_compound, Thrombin, Polysaccharides, medicine, Humans, Thrombophilia, Molecular Biology, Protein C Inhibitor, Serine protease, Protease, biology, Heparin, Cell Biology, Atherosclerosis, Protein Structure, Tertiary, carbohydrates (lipids), chemistry, Conventional PCI, biology.protein, medicine.drug

Abstract

Protein C inhibitor (PCI) is a serine protease inhibitor, displaying broad protease specificity, found in blood and other tissues. In blood, it is capable of inhibiting both procoagulant and anticoagulant proteases. Mechanisms that provide specificity to PCI remain largely unrevealed. In this study we have for the first time provided a full explanation for the marked size heterogeneity of blood-derived PCI and identified functional differences between naturally occurring PCI variants. The heterogeneity was caused by differences in N-glycan structures, N-glycosylation occupancy, and the presence of a Delta6-N-cleaved form. Bi-, tri-, and tetra-antennary complex N-glycans were identified. Fucose residues were identified both on the core GlcNAc and as parts of sialyl-Le(a/x) epitopes. Moreover, a glycan with a composition that implied a di-sialyl antenna was observed. PCI was N-glycosylated at all three potential N-glycosylation sites, Asn-230, Asn-243, and Asn-319, but a small fraction of PCI lacked the N-glycan at Asn-243. The overall removal of N-glycans affected the maximal heparin- and thrombomodulin-enhanced rates of thrombin inhibition differently in different solution conditions. In contrast, the Delta6-N-region increased both the heparin- and the thrombomodulin-enhanced rates of thrombin inhibition at all conditions examined. These results thus demonstrate that the N-linked glycans and the N-terminal region of blood-derived PCI in different ways affect the cofactor-enhanced rates of thrombin inhibition and provide information on the mechanisms by which this may be achieved. The findings are medically important, in view of the documented association of PCI with atherosclerotic plaques and the promising effect of PCI on reducing hypercoagulability states.

Published

2008

29. Molecular basis of thrombin recognition by protein C inhibitor revealed by the 1.6-Å structure of the heparin-bridged complex

Author

James A. Huntington, Charles T. Esmon, Ty E. Adams, Jyoti Nangalia, and Wei Li

Subjects

Models, Molecular, Thrombomodulin, Protein C inhibitor, Serpin, Crystallography, X-Ray, Protein Structure, Secondary, Protein structure, Thrombin, medicine, Humans, cardiovascular diseases, Reactive center, Protein C Inhibitor, Multidisciplinary, Heparin, Chemistry, Biological Sciences, surgical procedures, operative, Biochemistry, Mutagenesis, Conventional PCI, therapeutics, medicine.drug

Abstract

Protein C inhibitor (PCI) is a serpin with many roles in biology, including a dual role as pro- and anticoagulant in blood. The protease specificity and local function of PCI depend on its interaction with cofactors such as heparin-like glycosaminoglycans (GAGs) and thrombomodulin (TM). Both cofactors significantly increase the rate of thrombin inhibition, but GAGs serve to promote the anticoagulant activity of PCI, and TM promotes its procoagulant function. To gain insight into how PCI recognition of thrombin is aided by these cofactors, we determined a crystallographic structure of the Michaelis complex of PCI, thrombin, and heparin to 1.6 Å resolution. Thrombin interacts with PCI in an unusual fashion that depends on the length of PCI's reactive center loop (RCL) to align the heparin-binding sites of the two proteins. The principal exosite contact is engendered by movement of thrombin's 60-loop in response to the unique P2 Phe of PCI. This mechanism of communication between the active site of thrombin and its recognition exosite is previously uncharacterized and may relate to other thrombin substrate–cofactor interactions. The cofactor activity of heparin thus depends on the formation of a heparin-bridged Michaelis complex and substrate-induced exosite contacts. We also investigated the cofactor effect of TM, establishing that TM bridges PCI to thrombin through additional direct interactions. A model of the PCI–thrombin–TM complex was built and evaluated by mutagenesis and suggests distinct binding sites for heparin and TM on PCI. These data significantly improve our understanding of the cofactor-dependent roles of PCI in hemostasis.

Published

2008

30. Insulin Resistance Is Unrelated to Circulating Retinol Binding Protein and Protein C Inhibitor

Author

Oswald Wagner, Peter Nowotny, Jelena Todoric, Michael Krebs, Martin G. Bischof, Anton Luger, Harald Esterbauer, Miriam Promintzer, and Christian Anderwald

Subjects

Blood Glucose, Male, Aging, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, Protein C inhibitor, medicine.medical_treatment, Blotting, Western, Clinical Biochemistry, Retinol transport, Enzyme-Linked Immunosorbent Assay, Context (language use), Fatty Acids, Nonesterified, Biology, Biochemistry, Gas Chromatography-Mass Spectrometry, Body Mass Index, Endocrinology, Insulin resistance, Internal medicine, medicine, Humans, Insulin, Vitamin A, Protein C Inhibitor, Sex Characteristics, C-Peptide, Body Weight, Biochemistry (medical), Middle Aged, Glucose clamp technique, medicine.disease, Retinol binding protein, Glucose Clamp Technique, Female, Insulin Resistance, Retinol binding, Retinol-Binding Proteins, Plasma

Abstract

Context: Recent data suggest that circulating retinol-binding protein (RBP) might be involved in the pathogenesis of insulin resistance. Moreover, protein C inhibitor (PCI), which specifically binds retinoic acid, was found to be increased in myocardial infarction survivors who are also insulin resistant.Objective: The objective of this study was to investigate the association of insulin resistance with RBP factors and PCI active antigen.Design and Setting: This was a clinical study.Patients: Nondiabetic humans with high (IS; n = 20, 14 females, six males, aged 47.2 ± 1.9 yr, body mass index 26 ± 1 kg/m2) and low (IR; n = 20, 14 females, six males, aged 45.5 ± 1.7 yr, body mass index 28 ± 1 kg/m2) insulin-stimulated glucose-disposal (M) participated in this study.Main Outcome Measures: M was measured by 2-h hyperinsulinemic (40 mU·min−1·m−2)-isoglycemic clamp tests. Measurements of RBP were performed using a nephelometric method and validated using quantitative Western blotting.Results: M (80–120 min) was higher in IS (10.9 ± 0.6 mg·min−1·kg−1) than IR (4.0 ± 0.2; P < 10−12). Fasting plasma RBP concentrations were comparable between IS and IR measured by both nephelometry (IS: 4.4 ± 0.3; IR: 4.6 ± 0.3 mg/dl, P = 0.6) and quantitative Western blot (IS 7.9 ± 0.5, IR 8.3 ± 0.6 mg/dl; P = 0.6). Fasting plasma PCI active antigen was similar in both groups. Plasma RBP and PCI were not significantly related to M. RBP was positively correlated with uric acid (r = 0.488, P = 0.003), triglycerides (r = 0.592, P < 0.001), prealbumin (r = 0.63, P < 0.0001), and vitamin A (r = 0.75, P < 10−6).Conclusions: Our data demonstrate that healthy, insulin-resistant humans do not show altered plasma retinol binding factors, such as RBP and PCI. Both do not significantly correlate with insulin sensitivity. Thus, our findings do not support the hypothesis of insulin sensitivity modulation by proteins involved in retinol transport.

Published

2007

31. Serpins in thrombosis, hemostasis and fibrinolysis

Author

Lea M. Beaulieu, Jill C. Rau, Frank C. Church, and James A. Huntington

Subjects

Heparin cofactor II, Hemostasis, Proteases, animal structures, Fibrinolysis, medicine.medical_treatment, Protein C inhibitor, Antithrombin, Thrombosis, Hematology, Article, Protease inhibitor (biology), Cell biology, carbohydrates (lipids), chemistry.chemical_compound, Biochemistry, chemistry, Plasminogen activator inhibitor-1, medicine, Humans, Plasminogen activator, Serpins, medicine.drug

Abstract

Hemostasis and fibrinolysis, the biological processes that maintain proper blood flow, are the consequence of a complex series of cascading enzymatic reactions. Serine proteases involved in these processes are regulated by feedback loops, local cofactor molecules, and serine protease inhibitors (serpins). The delicate balance between proteolytic and inhibitory reactions in hemostasis and fibrinolysis, described by the coagulation, protein C and fibrinolytic pathways, can be disrupted, resulting in the pathological conditions of thrombosis or abnormal bleeding. Medicine capitalizes on the importance of serpins, using therapeutics to manipulate the serpin-protease reactions for the treatment and prevention of thrombosis and hemorrhage. Therefore, investigation of serpins, their cofactors, and their structure-function relationships is imperative for the development of state-of-the-art pharmaceuticals for the selective fine-tuning of hemostasis and fibrinolysis. This review describes key serpins important in the regulation of these pathways: antithrombin, heparin cofactor II, protein Z-dependent protease inhibitor, alpha(1)-protease inhibitor, protein C inhibitor, alpha(2)-antiplasmin and plasminogen activator inhibitor-1. We focus on the biological function, the important structural elements, their known non-hemostatic roles, the pathologies related to deficiencies or dysfunction, and the therapeutic roles of specific serpins.

Published

2007

32. Regulation of protein C inhibitor (PCI) activity by specific oxidized and negatively charged phospholipids

Author

Ingrid Jerabek, Julia M. Malleier, Valery N. Bochkov, Bernd R. Binder, Thomas Perkmann, Johannes M. Breuss, Margarethe Geiger, Olga Oskolkova, and Barbora Sokolikova

Subjects

Protein C inhibitor, Immunology, Phospholipid, Tretinoin, Phosphatidylserines, Serpin, Biochemistry, chemistry.chemical_compound, Annexin, medicine, Humans, cardiovascular diseases, Annexin A5, Phospholipids, Protein C Inhibitor, Phosphatidylethanolamine, Dose-Response Relationship, Drug, Heparin, Cell Biology, Hematology, Phosphatidylserine, Atherosclerosis, Lipids, Molecular biology, Recombinant Proteins, Oxygen, surgical procedures, operative, Gene Expression Regulation, chemistry, Conventional PCI, Calcium, therapeutics, Protein C, Protein Binding, medicine.drug

Abstract

Protein C inhibitor (PCI) is a serpin with affinity for heparin and phosphatidylethanolamine (PE). We analyzed the interaction of PCI with different phospholipids and their oxidized forms. PCI bound to oxidized PE (OxPE), and oxidized and unoxidized phosphatidylserine (PS) immobilized on microtiter plates and in aqueous suspension. Binding to OxPE and PS was competed by heparin, but not by the aminophospholipid-binding protein annexin V or the PCI-binding lipid retinoic acid. PS and OxPE stimulated the inhibition of activated protein C (aPC) by PCI in a Ca++-dependent manner, indicating that binding of both, aPC (Ca++ dependent) and PCI (Ca++ independent), to phospholipids is necessary. A peptide corresponding to the heparin-binding site of PCI abolished the stimulatory effect of PS on aPC inhibition. No stimulatory effect of phospholipids on aPC inhibition was seen with a PCI mutant lacking the heparin-binding site. A heparin-like effect of phospholipids (OxPE) was not seen with antithrombin III, another heparin-binding serpin, suggesting that it is specific for PCI. PCI and annexin V were found to be endogenously colocalized in atherosclerotic plaques, supporting the hypothesis that exposure of oxidized PE and/or PS may be important for the local regulation of PCI activity in vivo.

Published

2007

33. Role of Protein C Inhibitor and Tissue Factor in Fertilization

Author

José A. Fernández and Mary J. Heeb

Subjects

Male, Serine protease, endocrine system, biology, urogenital system, Protein C inhibitor, Seminal Plasma Proteins, Semen, Hematology, Kallikrein, Sperm, Thromboplastin, Tissue factor, fluids and secretions, Coagulation, Biochemistry, Fertilization, biology.protein, Humans, Female, Cardiology and Cardiovascular Medicine, Protein C

Abstract

Semen coagulation is achieved by a series of biochemical processes designed to protect and guide the sperm during its migration through the female genital tract so that spermatozoa reach the ovum successfully. Thus, semen coagulation promotes fertilization. The mechanism of semen coagulation is similar in principle to blood coagulation and fibrinolysis because it requires the catalytic activity of proteases to convert a soluble substrate to an insoluble gel, and then dissolve the gel over a longer period of time. In fact, there are traces of most blood coagulation factors and fibrinolytic factors in semen; the roles of these factors in semen coagulation are still to be determined. This review focuses on two such proteins that have remarkably high levels in semen: protein C inhibitor and tissue factor. Protein C inhibitor is a serine protease inhibitor that modulates the activity of several blood-clotting factors and activated protein C. Tissue factor (thromboplastin) is a membrane protein crucial for the initiation of the extrinsic cascade of blood coagulation. The emerging roles of these two proteins in semen coagulation and in fertilization processes are summarized.

Published

2007

34. The Interaction among Protein C Inhibitor, Prostate-Specific Antigen, and the Semenogelin System

Author

Junji Nishioka, Koji Suzuki, Tatsuya Hayashi, and Hideaki Kise

Subjects

Male, Protein C inhibitor, Semen, Seminal Vesicle Secretory Proteins, urologic and male genital diseases, Humans, cardiovascular diseases, Ternary complex, Protein C Inhibitor, Serine protease, biology, Vesicle, Seminal Vesicles, Hematology, Hydrogen-Ion Concentration, Prostate-Specific Antigen, Zinc, Prostate-specific antigen, surgical procedures, operative, Biochemistry, Multiprotein Complexes, Conventional PCI, biology.protein, Cardiology and Cardiovascular Medicine, therapeutics, Semenogelin, Protein Binding

Abstract

The kallikrein-like serine protease, prostate-specific antigen (PSA), is mixed in human seminal plasma with its protein substrates semenogelin (Sg) -I, Sg-II, and protein C inhibitor (PCI), which are produced in seminal vesicles. In the seminal plasma, PSA degrades Sg-I, and Sg-II, which are major components in insoluble coagula, and PCI inhibits PSA by forming a PSA-PCI complex. Digestion of seminal coagula with PSA releases PCI and PSA-PCI complex from the coagula into a soluble phase, suggesting the presence of active PCI within the coagula. PCI forms a ternary complex with PSA and Sg-II in the seminal plasma. The binding of Sg-II to PSA and PCI is influenced by pH, ionic strength, heparin, negatively charged dextran sulfate, divalent cations, and particularly by Zn 2 +. These observations suggest that binding of PCI to Sg in seminal vesicles regulates the PSA-catalyzed degradation of Sg in seminal plasma; the complex formation among PCI, PSA, and Sg is modulated by several factors in seminal plasma.

Published

2007

35. Characterization of recombinant human protein C inhibitor expressed in Escherichia coli

Author

Julia M. Malleier, Yolanda M. Fortenberry, Frank C. Church, Scott T. Cooper, Sophie M. Réhault, Margareta Zechmeister-Machhart, Margarethe Geiger, and Nikki M. Binz

Subjects

Proteases, Serine Proteinase Inhibitors, Protein C inhibitor, Molecular Sequence Data, Biophysics, Serpin, Biochemistry, Analytical Chemistry, law.invention, Thrombin, Affinity chromatography, law, Escherichia coli, medicine, Humans, Amino Acid Sequence, Molecular Biology, Protein C Inhibitor, Serine protease, biology, Heparin, Urokinase-Type Plasminogen Activator, Molecular biology, Recombinant Proteins, Mutation, biology.protein, Recombinant DNA, Sequence Alignment, Plasminogen activator, Protein C, medicine.drug

Abstract

The serine protease inhibitor (serpin) protein C inhibitor (PCI; also named plasminogen activator inhibitor-3) regulates serine proteases in hemostasis, fibrinolysis, and reproduction. The biochemical activity of PCI is not fully defined partly due to the lack of a convenient expression system for active rPCI. Using pET-15b plasmid, Ni(2+)-chelate and heparin-Sepharose affinity chromatography steps, we describe here the expression, purification and characterization of wild-type recombinant (wt-rPCI) and two inactive mutants, R354A (P1 residue) and T341R (P14 residue), expressed in Escherichia coli. Wild-type rPCI, but not the two mutants, formed a stable bimolecular complex with thrombin, activated protein C and urokinase. In the absence of heparin, wt-rPCI-thrombin, -activated protein C, and -urokinase inhibition rates were 56.7, 3.4, and 2.3 x 10(4) M(-1) min(-1), respectively, and the inhibition rates were accelerated 25-, 71-, and 265-fold in the presence of 10 mug/mL heparin for each respective inhibition reaction. The stoichiometry of inhibition (SI) for wt-rPCI-thrombin was 2.0, which is comparable to plasma-derived PCI. The present report describes for the first time the expression and characterization of recombinant PCI in a bacterial expression system and demonstrates the feasibility of using this system to obtain adequate amounts of biologically active rPCI for future structure-function studies.

Published

2005

36. Mechanisms of glycosaminoglycan activation of the serpins in hemostasis

Author

James A. Huntington

Subjects

Models, Molecular, Protein Conformation, Plasmin, Thrombomodulin, Protein C inhibitor, Molecular Sequence Data, Biology, Serpin, chemistry.chemical_compound, Thrombin, medicine, Animals, Humans, Serpins, Glycosaminoglycans, Protein C Inhibitor, Heparin cofactor II, Hemostasis, Antithrombin, Hematology, Protein Structure, Tertiary, carbohydrates (lipids), Carbohydrate Sequence, Models, Chemical, Biochemistry, chemistry, Plasminogen activator inhibitor-1, Factor Xa, medicine.drug

Abstract

Serpins are the predominant protease inhibitors in the higher organisms and are responsible, in humans, for the control of many highly regulated processes including blood coagulation and fibrinolysis. The serpin inhibitory mechanism has recently been revealed by the solution of a crystallographic structure of the final serpin-protease complex. The serpin mechanism, in contrast to the classical lock-and-key mechanism, involves dramatic conformational change in both the inhibitor and the inhibited protein. The final result is a stable covalent complex in which the properties of each component are altered so as to allow clearance from the circulation. Several serpins are involved in hemostasis: antithrombin (AT) inhibits many coagulation proteases, most importantly factor Xa and thrombin; heparin cofactor II (HCII) inhibits thrombin; protein C inhibitor (PCI) inhibits activated protein C and thrombin bound to thrombomodulin; plasminogen activator inhibitor 1 inhibits tissue plasminogen activator; and alpha2-antiplasmin inhibits plasmin. Nearly all of these reactions are accelerated through interactions with glycosaminoglycans (GAGs) such as heparin or heparan sulfate. Recent structures of AT, HCII and PCI have revealed how in each case the serpin mechanism has been fine-tuned by evolution to bring about high levels of regulatory control, and how seemingly disparate mechanisms of GAG binding and activation can share critical elements. By considering the serpins involved in hemostasis together it is possible to develop a deeper understanding of their complex individual roles.

Published

2003

37. Basic residues in the 37-loop of activated protein C modulate inhibition by protein C inhibitor but not by α1-antitrypsin

Author

Laura N. Glasscock, Frank C. Church, Brian W. Grinnell, Bruce Gerlitz, and Scott T. Cooper

Subjects

Models, Molecular, Serine Proteinase Inhibitors, Protein Conformation, Protein C inhibitor, Biophysics, Serpin, Biochemistry, Analytical Chemistry, law.invention, Plasma, Structure-Activity Relationship, law, medicine, Humans, Molecular Biology, Protein C Inhibitor, Serine protease, Binding Sites, Chymotrypsin, biology, Heparin, Chemistry, Lysine, Molecular biology, Recombinant Proteins, alpha 1-Antitrypsin, Mutation, Mutagenesis, Site-Directed, Recombinant DNA, biology.protein, Plasminogen activator, Protein C, medicine.drug

Abstract

The role of lysines 37-39 (chymotrypsin numbering) in the 37-loop of the serine protease activated protein C (APC) was studied by expressing acidic and neutral recombinant APC (rAPC) mutants. Activity of the APC mutants was assessed using human plasma and plasma-purified and recombinant derivatives of protein C inhibitor (PCI; also known as plasminogen activator inhibitor-3) and alpha(1)-antitrypsin, with and without heparin. The catalytic properties of the mutants to small peptidyl substrates were essentially the same as wild-type rAPC (wt-rAPC), yet their plasma anticoagulant activities were diminished. Analysis of the rAPC-protease inhibitor complexes formed after addition of wt-rAPC and mutants to plasma revealed no change in the inhibition pattern by alpha(1)-antitrypsin but a reduction in mutant complex formation by PCI in the presence of heparin. Using purified serpins, we found that inhibition rates of the mutants were the same as wt-rAPC with alpha(1)-antitrypsin; however, PCI (plasma-derived and recombinant forms) inhibition rates of the acidic mutants were slightly faster than that of wt-rAPC without heparin. By contrast, PCI-heparin inhibition rates of the mutants were not substantially accelerated compared to wt-rAPC. The mutants had reduced heparin-binding properties compared to wt-rAPC. Molecular modeling of the PCI-APC complex with heparin suggests that heparin may function not only to bridge PCI to APC, but also to alleviate putative non-optimal intermolecular interactions. Our results suggest that the basic residues of the 37-loop of APC are involved in macromolecular substrate interactions and in heparin binding, and they influence inhibition by PCI (with or without heparin) but not by alpha(1)-antitrypsin, two important blood plasma serpins.

Published

2003

38. Crystal Structure of Protein C Inhibitor Provides Insights into Hormone Binding and Heparin Activation

Author

James A. Huntington, Margareta Kjellberg, and Johan Stenflo

Subjects

Retinoid binding, Protein C inhibitor, Plasma protein binding, 030204 cardiovascular system & hematology, Serpin, Crystallography, X-Ray, Protein Structure, Secondary, Retinoids, 03 medical and health sciences, 0302 clinical medicine, Protein structure, Structural Biology, Binding site, Molecular Biology, Reactive center, Protein C Inhibitor, 030304 developmental biology, 0303 health sciences, Binding Sites, Heparin, Chemistry, serpin, protease, thrombin, Protein Structure, Tertiary, inhibitor, Biochemistry, retinoid, Docking (molecular), Biophysics, Protein Binding

Abstract

Protein C inhibitor (PCI) is a member of the serpin family that has many biological functions. In blood it acts as a procoagulant, and, in the seminal vesicles, it is required for spermatogenesis. The activity of PCI is affected by heparin binding in a manner unique among the heparin binding serpins, and, in addition, PCI binds hydrophobic hormones with apparent specificity for retinoids. Here we present the 2.4 Å crystallographic structure of reactive center loop (RCL) cleaved PCI. A striking feature of the structure is a two-turn N-terminal shortening of helix A, which creates a large hydrophobic pocket that docking studies indicate to be the retinoid binding site. On the basis of surface electrostatic properties, a novel mechanism for heparin activation is proposed.

Published

2003

39. Exosite-Dependent Regulation of the Protein C Anticoagulant Pathway

Author

Alireza R. Rezaie

Subjects

Serine protease, Binding Sites, biology, Chemistry, Protein C inhibitor, Anticoagulants, Plasma protein binding, APC/C activator protein CDH1, Thrombin, Biochemistry, Zymogen, medicine, biology.protein, Humans, Cardiology and Cardiovascular Medicine, Blood Coagulation, Plasminogen activator, Protein C, Protein Binding, Signal Transduction, medicine.drug

Abstract

Activated protein C (APC) is a vitamin K-dependent anticoagulant serine protease in plasma that downregulates the coagulation cascade by degrading cofactors Va and VIIIa by limited proteolysis. In addition to its anticoagulant function, APC also exhibits potent profibrinolytic and anti-inflammatory properties. The proteolytic activity of APC in plasma is slowly inhibited by three serpins: protein C inhibitor, plasminogen activator inhibitor-1, and alpha(1)-antitrypsin. Recent structural and mutagenesis data have indicated that basic residues of three exposed surface loops known as the 39-loop (Lys(37)-Lys(39)), 60-loop (Lys(62), Lys(63)), and 70-80-loop (Arg(74), Arg(75), and Lys(78)) (chymotrypsin numbering) constitute an anion-binding exosite in APC that interacts with these macromolecular substrates and inhibitors. Moreover, this exosite plays a critical role in the thrombomodulin-dependent activation of the zymogen protein C by thrombin. This article briefly reviews how the binding of physiological protein and polysaccharide cofactors on this exosite modulates the protein C anticoagulant pathway in plasma.

Published

2003

40. Substrate specificity of human kallikrein 2 (hK2) as determined by phage display technology

Author

JeanâPierre Mach, Jair R. Chagas, Cloutier Sylvain, Christian M. Gygi, David Deperthes, and HansâJurg Leisinger

Subjects

Serine protease, Phage display, Biochemistry, Protein C inhibitor, biology.protein, Tissue Kallikreins, Kallikrein, Biology, Peptide library, Molecular biology, Pentapeptide repeat, Green fluorescent protein

Abstract

Human glandular kallikrein 2 (hK2) is a trypsin-like serine protease expressed predominantly in the prostate epithelium. Recently, hK2 has proven to be a useful marker that can be used in combination with prostate specific antigen for screening and diagnosis of prostate cancer. The cleavage by hK2 of certain substrates in the proteolytic cascade suggest that the kallikrein may be involved in prostate cancer development; however, there has been very little other progress toward its biochemical characterization or elucidation of its true physiological role. In the present work, we adapt phage substrate technology to study the substrate specificity of hK2. A phage-displayed random pentapeptide library with exhaustive diversity was generated and then screened with purified hK2. Phages displaying peptides susceptible to hK2 cleavage were amplified in eight rounds of selection and genes encoding substrates were transferred from the phage to a fluorescent system using cyan fluorescent protein (derived from green fluorescent protein) that enables rapid determination of specificity constants. This study shows that hK2 has a strict preference for Arg in the P1 position, which is further enhanced by a Ser in P'1 position. The scissile bonds identified by phage display substrate selection correspond to those of the natural biological substrates of hK2, which include protein C inhibitor, semenogelins, and fibronectin. Moreover, three new putative hK2 protein substrates, shown elsewhere to be involved in the biology of the cancer, have been identified thus reinforcing the importance of hK2 in prostate cancer development.

Published

2002

41. Contribution of Basic Residues of the 70−80-Loop to Heparin Binding and Anticoagulant Function of Activated Protein C

Author

Chandrashekhara Manithody, Likui Yang, and Alireza R. Rezaie

Subjects

Models, Molecular, Stereochemistry, Protein C inhibitor, Mutant, In Vitro Techniques, Biochemistry, Thrombin, medicine, Humans, Ternary complex, Protein C Inhibitor, chemistry.chemical_classification, Binding Sites, Chymotrypsin, biology, Chemistry, Heparin, Oligosaccharide, Recombinant Proteins, Protein Structure, Tertiary, Kinetics, Amino Acid Substitution, Mutagenesis, Site-Directed, biology.protein, Protein C, medicine.drug

Abstract

The role of basic residues of the 70-80-loop, Arg(74), Arg(75), and Lys(78) (chymotrypsin numbering) in the catalytic function of activated protein C (APC) was investigated by expressing mutants of protein C in which these residues were replaced with Ala in three separate constructs. Following purification to homogeneity and activation by thrombin, the catalytic properties of the mutants were characterized with respect to their ability to cleave the chromogenic substrate Spectrozyme PCa, react with protein C inhibitor (PCI), and inactivate factor Va. Relative to wild-type APC, the mutants cleaved Spectrozyme PCa with identical or improved catalytic efficiencies. Similarly, PCI inhibited mutants with identical or improved second-order rate constants (k(2)) in the absence of heparin. However, the heparin-catalyzed inhibition of mutants by PCI was impaired approximately 10-fold. Analysis of k(2) values by a ternary complex model revealed that the affinities of mutants for heparin were impaired to a similar extent. Moreover, analysis of the NaCl gradient elution profiles of APC derivatives from Heparin-Sepharose supported this conclusion. An oligosaccharide containing 14 residues efficiently catalyzed the PCI inhibition of APC by a template mechanism. Further studies revealed that the ability of Arg(74) and Arg(75) mutants to inactivate factor Va was markedly impaired. We conclude that basic residues of the 70-80-loop are critical for the catalytic function of APC.

Published

2002

42. 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

43. Protein C and Protein S Deficiencies

Author

Sébastien Humbert and Philippe Humbert

Subjects

biology, Chemistry, Protein C inhibitor, Thrombomodulin, medicine.disease, Cofactor, Protein S, Thrombin, Coagulation, Biochemistry, biology.protein, medicine, Protein C, medicine.drug, Purpura fulminans

Abstract

Protein C and protein S are vitamin K-dependent protein with natural anticoagulant properties that play a major role in the coagulation pathway. Protein C is activated by the thrombin/thrombomodulin complex. Activated protein C cleaves membrane-bound active factors V and VIII and inactivates them. Protein C inhibitor and α-1 antitrypsin are the main inhibitors of protein C. Protein S is a cofactor of activated protein C and can also directly bond to activated factors V and X.

Published

2014

44. Identification of the Protein C/Activated Protein C Binding Sites on the Endothelial Cell Protein C Receptor

Author

Timothy Mather, Natalia Oganesyan, Charles T. Esmon, Gary L. Ferrell, and Patricia C. Liaw

Subjects

biology, Binding protein, Protein C inhibitor, Cell Biology, Ligand (biochemistry), Biochemistry, Molecular biology, Fusion protein, Epitope, Transmembrane protein, MHC class I, biology.protein, Binding site, Molecular Biology

Abstract

The endothelial cell protein C receptor (EPCR) is an endothelial cell-specific transmembrane protein that binds both protein C and activated protein C (APC). EPCR regulates the protein C anticoagulant pathway by binding protein C and augmenting protein C activation by the thrombin-thrombomodulin complex. EPCR is homologous to the MHC class 1/CD1 family, members of which contain two α-helices that sit upon an 8-stranded β-sheet platform. In this study, we identified 10 residues that, when mutated to alanine, result in the loss of protein C/APC binding (Arg-81, Leu-82, Val-83, Glu-86, Arg-87, Phe-146, Tyr-154, Thr-157, Arg-158, and Glu-160). Glutamine substitutions at the four N-linked carbohydrate attachment sites of EPCR have little affect on APC binding, suggesting that the carbohydrate moieties of EPCR are not critical for ligand recognition. We then mapped the epitopes for four anti-human EPCR monoclonal antibodies (mAbs), two of which block EPCR/Fl-APC (APC labeled at the active site with fluorescein) interactions, whereas two do not. These epitopes were localized by generating human-mouse EPCR chimeric proteins, since the mAbs under investigation do not recognize mouse EPCR. We found that 5 of the 10 candidate residues for protein C/APC binding (Arg-81, Leu-82, Val-83, Glu-86, Arg-87) colocalize with the epitope for one of the blocking mAbs. Three-dimensional molecular modeling of EPCR indicates that the 10 protein C/APC binding candidate residues are clustered at the distal end of the two α-helical segments. Protein C activation studies on 293 cells that coexpress EPCR variants and thrombomodulin demonstrate that protein C binding to EPCR is necessary for the EPCR-dependent enhancement in protein activation by the thrombin-thrombomodulin complex. These studies indicate that EPCR has exploited the MHC class 1 fold for an alternative and possibly novel mode of ligand recognition. These studies are also the first to identify the protein C/APC binding region of EPCR and may provide useful information about molecular defects in EPCR that could contribute to cardiovascular disease susceptibility.

Published

2001

45. Protein C Inhibitor Regulates the Thrombin-Thrombomodulin Complex in the Up- and Down Regulation of TAFI Activation

Author

Joost C. M. Meijers, Marc G L M Elisen, Bonno N. Bouma, and Laurent O. Mosnier

Subjects

chemistry.chemical_classification, biology, Protein C inhibitor, medicine.medical_treatment, Hematology, Thrombomodulin, Molecular biology, Carboxypeptidase, Enzyme, Thrombin, chemistry, Coagulation, Biochemistry, Fibrinolysis, medicine, biology.protein, Protein C, medicine.drug

Abstract

SummaryThrombin Activatable Fibrinolysis Inhibitor (TAFI) is a carboxypeptidase B-like proenzyme that after activation by thrombin down regulates fibrinolysis. Thrombomodulin (TM) stimulates the activation of both TAFI and protein C whereas activated protein C (APC) inhibits the activation of TAFI by down regulating thrombin generation. Recently, protein C inhibitor (PCI) was identified as a potent inhibitor of thrombin bound to TM and it can thereby regulate the balance between TAFI activation, and inhibition of TAFI activation by APC. Both in a purified system and in plasma, activation of TAFI and protein C by IIa-TM could be inhibited by PCI. Previously we found in plasma that at low concentrations (~1 nM), TM predominantly stimulated the activation of TAFI whereas at higher concentrations of TM (~10 nM) the activation of protein C resulted in inhibition of the activation of TAFI. In agreement with this, PCI inhibited the activation of TAFI at 1 nM TM whereas at 10 nM TM PCI inhibited the activation of protein C resulting in an increase in the activation of TAFI. This suggests that PCI can up regulate TAFI activation by inhibiting the protein C activation. PCI may therefore be an important regulator in the balance between coagulation and fibrinolysis by differentially inhibiting the activation of TAFI and of protein C. The local TM concentration plays an important role in the outcome of this process.

Published

2001

46. Tracking Structural Features Leading to Resistance of Activated Protein C to α1-antitrypsin

Author

Björn Dahlbäck, Bruno O. Villoutreix, and Lei Shen

Subjects

Models, Molecular, congenital, hereditary, and neonatal diseases and abnormalities, Surface Properties, Mutant, Drug Resistance, Serpin, Biochemistry, Catalysis, law.invention, Structure-Activity Relationship, law, medicine, Animals, Humans, Activated Protein C Resistance, Protein C Inhibitor, Serine protease, chemistry.chemical_classification, biology, Heparin, Mutagenesis, Anticoagulants, Molecular biology, Recombinant Proteins, Amino acid, Enzyme Activation, Enzyme, chemistry, alpha 1-Antitrypsin, Mutagenesis, Site-Directed, Recombinant DNA, biology.protein, Cattle, Protein C, Protein Binding, medicine.drug

Abstract

Activated protein C (APC) is a multi-modular anticoagulant serine protease, which degrades factor V/Va and factor VIIIa. Human APC (hAPC) is inhibited by human alpha 1-antitrypsin (AAT), while the bovine enzyme (bAPC) is fully resistant to this serpin. Structural features in the catalytic domains between the two species cause this difference, but detailed knowledge about the causal molecular difference is missing. To gain insight into the APC-AAT interaction and to create a human protein C resistant to AAT inhibition, we have used molecular modeling and site-directed mutagenesis. First, a structural model for bAPC based on the Gla-domainless X-ray structure of hAPC was built. Screening the molecular surface of the human and bovine APC enzymes suggested that a hAPC molecule resistant to AAT inhibition could be constructed by substituting only a few amino acids. We thus produced recombinant hAPC molecules with a single mutation (S173E, the numbering follows the chymotrypsinogen nomenclature), two mutations (E60aS/S61R) or a combination of all these substitutions (E60aS/S61R/S173E). Amidolytic and anticoagulant activities of the three mutant APC molecules were similar to those of wild-type hAPC. Inhibition of wild-type hAPC by AAT was characterized by a second-order rate constant (k2) of 2.71 M-1 s-1. The amino acid substitution at position 173 (S173E mutant) led to partial resistance to AAT (k2 = 0.84 M-1 s-1). The E60aS/S61R mutant displayed mild resistance to AAT inhibition (k2 = 1.70 M-1 s-1), whereas the E60aS/S61R/S173E mutant was inefficiently inactivated by AAT (k2 = 0.40 M-1 s-1). Inhibition of recombinant APC molecules by the serpin protein C inhibitor (PCI) in the presence and absence of heparin was also investigated.

Published

2000

47. Synthesis and Ultrastructural Localization of Protein C Inhibitor in Human Platelets and Megakaryocytes

Author

Johannes M. Breuss, Erika Vanyek-Zavadil, Maria J. Prendes, Veronica A. Carroll, Bernd R. Binder, Edith Bielek, Margareta Zechmeister-Machhart, and Margarethe Geiger

Subjects

Blood Platelets, media_common.quotation_subject, medicine.medical_treatment, Protein C inhibitor, Immunology, Cytoplasmic Granules, Biochemistry, Megakaryocyte, Fibrinolysis, medicine, Humans, Platelet, cardiovascular diseases, Microscopy, Immunoelectron, Internalization, Protein C Inhibitor, media_common, Gel electrophoresis, Chemistry, Cell Membrane, Cell Biology, Hematology, Immunohistochemistry, Molecular biology, Blot, medicine.anatomical_structure, surgical procedures, operative, Conventional PCI, Megakaryocytes, therapeutics, Plasminogen activator

Abstract

The occurrence of protein C inhibitor (PCI) in human platelets and megakaryocytes was analyzed. As judged from enzyme-linked immunosorbent assays (ELISAs), PCI was present in platelets at a concentration of 160 ng/2 × 109 cells. Its specific activity was 5 times higher than that of plasma PCI. Consistently, mainly the 57-kD form (active PCI) and some high molecular weight (Mr) forms, but no bands corresponding to cleaved PCI, were detected when platelet lysates were immunoprecipitated with monoclonal anti-PCI-IgG and analyzed by sodium dodecyl sulfate-polyacrylamide gel electrophoresis (SDS-PAGE) and Western blotting. The localization of PCI in platelets was studied by immunofluorescence histochemistry and immunotransmission electron microscopy: PCI was detected in  granules, in the open canalicular system, and on the plasma membrane. At these sites, colocalization with plasminogen activator inhibitor-1 was seen. Studies were performed to clarify whether platelet PCI is endogenously synthesized or taken up from plasma. Internalization of biotinylated-PCI was analyzed using platelets in suspension and gold-labeled streptavidin for visualization of incorporated biotin. Dose- and time-dependent uptake of PCI was found. PCI mRNA was detected in platelets by reverse transcriptase-polymerase chain reaction (RT-PCR) and Southern blotting, as well as in megakaryocytes by in situ hybridization of human bone marrow cryosections. We therefore conclude that platelets contain a functionally active PCI pool that is derived from both endogenous synthesis as well as internalization.

Published

1999

48. The Effect of Membrane Composition on the Hemostatic Balance

Author

M D Smirnov, Naomi L. Esmon, David A. Ford, and Charles T. Esmon

Subjects

chemistry.chemical_classification, Phosphatidylethanolamine, Chemistry, Phosphatidylethanolamines, Vesicle, Phospholipid, Fatty acid, Phosphatidylserines, Phosphatidylserine, Biochemistry, Membrane Lipids, chemistry.chemical_compound, Factor Va, Prothrombinase, Lupus Coagulation Inhibitor, Phosphatidylcholine, Phosphatidylcholines, medicine, Biophysics, Humans, Prothrombin, Blood Coagulation, Protein C, Protein C Inhibitor, medicine.drug

Abstract

The phospholipid composition requirements for optimal prothrombin activation and factor Va inactivation by activated protein C (APC) anticoagulant were examined. Vesicles composed of phosphatidylethanolamine (PE) and phosphatidylcholine (PC) supported factor Va inactivation relatively well. However, optimal factor Va inactivation still required relatively high concentrations of phosphatidylserine (PS). In addition, at a fixed concentration of phospholipid, PS, and APC, vesicles devoid of PE never attained a rate of factor Va inactivation achievable with vesicles containing PE. Polyunsaturation of any vesicle component also contributed significantly to APC inactivation of factor Va. Thus, PE makes an important contribution to factor Va inactivation that cannot be mimicked by PS. In the absence of polyunsaturation in the other membrane constituents, this contribution was dependent upon the presence of both the PE headgroup per se and unsaturation of the 1,2 fatty acids. Although PE did not affect prothrombin activation rates at optimal PS concentrations, PE reduced the requirement for PS approximately 10-fold. The Km(app) for prothrombin and the Kd(app) for factor Xa-factor Va decreased as a function of increasing PS concentration, reaching optimal values at 10-15% PS in the absence of PE but only 1% PS in the presence of PE. Fatty acid polyunsaturation had minimal effects. A lupus anticoagulant immunoglobulin was more inhibitory to both prothrombinase and factor Va inactivation in the presence of PE. The degree of inhibition of APC was significantly greater and much more dependent on the phospholipid composition than that of prothrombinase. Thus, subtle changes in the phospholipid composition of cells may control procoagulant and anticoagulant reactions differentially under both normal and pathological conditions.

Published

1999

49. α2-Macroglobulin and C1-Inactivator are Plasma Inhibitors of Human Glandular Kallikrein

Author

Francisco España and Mary J. Heeb

Subjects

Male, medicine.medical_treatment, Protein C inhibitor, Complement C1 Inactivator Proteins, Biomarkers, Tumor, medicine, Humans, alpha-Macroglobulins, Enzyme Inhibitors, Molecular Biology, Human Glandular Kallikrein, Protease, biology, Prostatic Neoplasms, Cell Biology, Hematology, Kallikrein, Macroglobulin, Biochemistry, Tissue Kallikreins, biology.protein, Molecular Medicine, Female, Kallikreins, Antibody

Abstract

Human glandular kallikrein (hK2) is a possible new marker for prostate cancer that is homologous to prostate specific antigen. Purified hK2 added to serum or plasma reacted with endogenous protease inhibitors to form complexes of >350, 135, and 80 kDa, and some hK2 remained free, as judged by immunoblotting. The former two complexes could be removed by specific antibodies to alpha2-macroglobulin and to C1- inactivator, respectively, and they comigrated on SDS-PAGE with complexes formed between hK2 and purified alpha2-macroglobulin or C1-inactivator. hK2 complexes of 80 kDa could not be completely removed with any anti-serpin antibody used. Thus, these may consist of more than one type of hK2 complex. In contrast, essentially all hK2 complexes were removed from seminal plasma by antibody to protein C inhibitor, demonstrating that protein C inhibitor is the only significant inhibitor of hK2 in semen. hK2 reacted more rapidly with alpha2-macroglobulin than with any other inhibitor in plasma or serum. Divalent metal ions and heparin did not appreciably affect the rate of formation of any of the hK2 complexes in serum or plasma or with purified alpha2-macroglobulin or C1-inactivator. Measurement of one or more of the hK2 forms identified here may have diagnostic or prognostic potential for prostate cancer.

Published

1998

50. Protein C Inhibitor Acts as a Procoagulant by Inhibiting the Thrombomodulin-Induced Activation of Protein C in Human Plasma

Author

M. G. L. M. Elisen, Bonno N. Bouma, P.A.K. von dem Borne, and Joost C. M. Meijers

Subjects

Chemistry, Protein C inhibitor, Immunology, Cell Biology, Hematology, Pharmacology, Thrombomodulin, Biochemistry, Tissue factor, surgical procedures, operative, Thrombin, Clotting time, Conventional PCI, medicine, Thromboplastin, cardiovascular diseases, therapeutics, Protein C, medicine.drug

Abstract

Protein C inhibitor (PCI), which was originally identified as an inhibitor of activated protein C, also efficiently inhibits coagulation factors such as factor Xa and thrombin. Recently it was found, using purified proteins, that the anticoagulant thrombin-thrombomodulin complex was also inhibited by PCI. The paradoxical inhibitory effect of PCI on both coagulant and anticoagulant proteases raised questions about the role of PCI in plasma. We studied the role of thrombomodulin (TM)-dependent inhibition of thrombin by PCI in a plasma system. Clotting was induced by addition of tissue factor to recalcified plasma in the absence or presence of TM, and clot formation was monitored using turbidimetry. In the absence of TM, PCI-deficient plasma showed a slightly shorter coagulation time compared with normal plasma. Reconstitution with a physiologic amount of PCI gave normal clotting times. Addition of PCI to normal plasma and protein C–deficient plasma resulted in a minor prolongation of the clotting time. This suggested that PCI can act as a weak coagulation inhibitor in the absence of TM. TM caused a strong anticoagulant effect in normal plasma due to thrombin scavenging and activation of the protein C anticoagulant pathway. This effect was less pronounced when protein C–deficient plasma was used, but could be restored by reconstitution with protein C. When PCI was added to protein C–deficient plasma in the presence of TM, a strong anticoagulant effect of PCI was observed. This anticoagulant effect was most likely caused by the TM-dependent thrombin inhibition by PCI. However, when PCI was added to normal plasma containing TM, a strong procoagulant effect of PCI was observed, due to the inhibition of protein C activation. PCI-deficient plasma was less coagulant in the presence of TM. A concentration-dependent increase in clotting time was observed when PCI-deficient plasma was reconstituted with PCI. The combination of these results suggest that the major function of PCI in plasma during coagulation is the inhibition of thrombin. A decreased generation of activated protein C is a procoagulant consequence of the TM-dependent thrombin inhibition by PCI. We conclude that TM alters PCI from an anticoagulant into a procoagulant during tissue factor-induced coagulation.

Published

1998