Your search keyword '"Factor XII Deficiency metabolism"' showing total 20 results

1. An update on factor XII-driven vascular inflammation.

Author

Mailer RK, Rangaswamy C, Konrath S, Emsley J, and Renné T

Subjects

Animals, Endothelium, Vascular pathology, Factor XII genetics, Humans, Inflammation, Angioedema metabolism, Atherosclerosis metabolism, Endothelium, Vascular metabolism, Factor XII metabolism, Factor XII Deficiency metabolism

Abstract

The plasma protein factor XII (FXII) is the liver-derived zymogen of the serine protease FXIIa that initiates an array of proteolytic cascades. Zymogen activation, enzymatic FXIIa activity and functions are regulated by interactions with cell receptors, negatively charged surfaces, other serine proteases, and serpin inhibitors, which bind to distinct protein domains and regions in FXII(a). FXII exerts mitogenic activity, while FXIIa initiates the pro-inflammatory kallikrein-kinin pathway and the pro-thrombotic intrinsic coagulation pathway, respectively. Growing evidence indicates that FXIIa-mediated thrombo-inflammation plays a crucial role in various pathological states besides classical thrombosis, such as endothelial dysfunction. Consistently, increased FXIIa levels are associated with hypercholesterolemia and hypertriglyceridemia. In contrast, FXII deficiency protects from thrombosis but is otherwise not associated with prolonged bleeding or other adverse clinical manifestations. Here, we review current concepts for FXII(a)-driven vascular inflammation focusing on endothelial hyperpermeability, receptor signaling, atherosclerosis and immune cell activation., (Copyright © 2021 Elsevier B.V. All rights reserved.)

Published

2022

2. Two Novel Mutations ( G774A and A1685G ) Causing Coagulation Factor XII Deficiency in a Patient with Acute Inferior Myocardial Infarction.

Author

Xiao B, Liu F, Jin YH, Wang MX, Zhang J, Lu JC, and Yang XC

Subjects

Factor XII Deficiency etiology, Factor XII Deficiency metabolism, Humans, Male, Middle Aged, Prognosis, Factor XII genetics, Factor XII Deficiency pathology, Inferior Wall Myocardial Infarction complications, Mutation

Abstract

Objective: To identify the gene mutation of the coagulation factor XII (FXII) in a patient with FXII deficiency and acute inferior myocardial infarction., Methods: The proband was a 51-year-old Chinese man who was diagnosed with acute inferior myocardial infarction and had a history of FXII deficiency. The patient presented with a prolonged activated partial thromboplastin time (160 s) and decreased FXII activity (2.3%) and FXII antigen (1%). DNA sequence analysis of the FXII gene was performed by next generation sequencing. The mutant FXII cDNAs were constructed in an expression plasmid vector and transfected into 293T cells. The expression of FXII antigen was detected by western blot., Results: Sequencing of the FXII gene revealed two novel heterozygous mutations, one at exon 8 (G774A; p: W258X) and the other at exon 14 (A1685G; p: D562G). Western blot showed that the FXII antigens were detected only in the supernatant and whole cell lysate of the wild-type and A1685G mutant type, but not in G774A or G774A plus the A1685G mutant type. In addition, the results showed that secretion but not synthesis of A1685G mutant protein was markedly reduced compared to the wild type., Conclusion: The present study indicated that the G774A mutation might impair the secretion and synthesis of FXII protein, while the A1685G mutation only influences the secretion of FXII protein. The definition of these new mutations could be useful tools for analyzing the intracellular protein transport and structure-function relationship of FXII protein transport in the future., (© 2021 by the Association of Clinical Scientists, Inc.)

Published

2021

3. Coagulation factor XII induces pro-inflammatory cytokine responses in macrophages and promotes atherosclerosis in mice.

Author

Vorlova S, Koch M, Manthey HD, Cochain C, Busch M, Chaudhari SM, Stegner D, Yepes M, Lorenz K, Nolte MW, Nieswandt B, and Zernecke A

Subjects

Animals, Antigen-Presenting Cells immunology, Aortic Diseases blood, Aortic Diseases genetics, Aortic Diseases immunology, Atherosclerosis blood, Atherosclerosis genetics, Atherosclerosis immunology, Cell Proliferation, Cytokines immunology, Disease Models, Animal, Factor XII genetics, Factor XII Deficiency blood, Factor XII Deficiency genetics, Factor XII Deficiency immunology, Factor XIIa genetics, Factor XIIa metabolism, Genetic Predisposition to Disease, Inflammation Mediators immunology, Lymphocyte Activation, Macrophages immunology, Mice, Inbred C57BL, Mice, Knockout, ApoE, Phenotype, Plaque, Atherosclerotic, Receptors, Urokinase Plasminogen Activator metabolism, Th1 Cells immunology, Th1 Cells metabolism, Time Factors, Antigen-Presenting Cells metabolism, Aortic Diseases metabolism, Atherosclerosis metabolism, Cytokines metabolism, Factor XII metabolism, Factor XII Deficiency metabolism, Inflammation Mediators metabolism, Macrophages metabolism

Abstract

Atherosclerosis is considered a chronic inflammatory disease of the vessel wall. Coagulation pathways and immune responses contribute to disease development. The role of coagulation factor XII (FXII) in vascular inflammation, however, remains controversial. We here investigated the function of FXII in atherosclerosis using apolipoprotein E and FXII-deficient (F12 -/- Apoe -/- ) mice. Compared to F12 +/+ Apoe -/- controls, atherosclerotic lesion formation was reduced in F12 -/- Apoe -/- mice. This was associated with a decrease in serum interleukin (IL)-1β and IL-12 levels and reduced expression of pro-inflammatory cytokines in the aorta in atherosclerotic F12 -/- Apoe -/- mice, as well as diminished Th1-cell differentiation in the aorta, blood, and lymphoid organs. No changes in circulating bradykinin, thrombin-antithrombin-complexes or plasminogen were observed. Mechanistically, activated FXII (FXIIa) was revealed to directly induce bone marrow-derived macrophages to secrete pro-inflammatory cytokines, including tumour necrosis factor-α, IL-1β, IL-12, and IL-6. Exposure of bone marrow-derived antigen presenting cells to FXIIa similarly induced pro-inflammatory cytokines, and an enhanced capacity to trigger antigen-specific interferon γ-production in CD4 + T cells. Notably, bone-marrow derived macrophages were capable of directly activating FXII. Moreover, the induction of cytokine expression by FXIIa in macrophages occurred independently of FXII protease enzymatic activity and was decreased upon phospholipase C treatment, suggesting urokinase-type plasminogen activator receptor (uPAR) to confer FXIIa-induced cell signalling. These data reveal FXII to play an important role in atherosclerotic lesion formation by functioning as a strong inducer of pro-inflammatory cytokines in antigen-presenting cells. Targeting of FXII may thus be a promising approach for treating cardiovascular disease.

Published

2017

4. Tissue factor-positive neutrophils bind to injured endothelial wall and initiate thrombus formation.

Author

Darbousset R, Thomas GM, Mezouar S, Frère C, Bonier R, Mackman N, Renné T, Dignat-George F, Dubois C, and Panicot-Dubois L

Subjects

Animals, Blood Coagulation, Blood Platelets cytology, Blood Vessels injuries, Blood Vessels metabolism, Blood Vessels pathology, Cell Adhesion, Cell Communication, Cell Count, Cell Movement, Endothelial Cells pathology, Endothelium, Vascular pathology, Factor XII metabolism, Factor XII Deficiency genetics, Factor XII Deficiency metabolism, Fibrin metabolism, Intercellular Adhesion Molecule-1 metabolism, Lasers, Mice, Monocytes cytology, Neutrophils cytology, Neutrophils transplantation, Platelet Count, Thromboplastin deficiency, Endothelial Cells metabolism, Endothelium, Vascular metabolism, Neutrophils metabolism, Thromboplastin genetics, Thrombosis metabolism

Abstract

For a long time, blood coagulation and innate immunity have been viewed as interrelated responses. Recently, the presence of leukocytes at the sites of vessel injury has been described. Here we analyzed interaction of neutrophils, monocytes, and platelets in thrombus formation after a laser-induced injury in vivo. Neutrophils immediately adhered to injured vessels, preceding platelets, by binding to the activated endothelium via leukocyte function antigen-1-ICAM-1 interactions. Monocytes rolled on a thrombus 3 to 5 minutes postinjury. The kinetics of thrombus formation and fibrin generation were drastically reduced in low tissue factor (TF) mice whereas the absence of factor XII had no effect. In vitro, TF was detected in neutrophils. In vivo, the inhibition of neutrophil binding to the vessel wall reduced the presence of TF and diminished the generation of fibrin and platelet accumulation. Injection of wild-type neutrophils into low TF mice partially restored the activation of the blood coagulation cascade and accumulation of platelets. Our results show that the interaction of neutrophils with endothelial cells is a critical step preceding platelet accumulation for initiating arterial thrombosis in injured vessels. Targeting neutrophils interacting with endothelial cells may constitute an efficient strategy to reduce thrombosis.

Published

2012

5. Factor XI and XII as antithrombotic targets.

Author

Müller F, Gailani D, and Renné T

Subjects

Animals, Anticoagulants therapeutic use, Blood Coagulation drug effects, Blood Coagulation physiology, Factor XI metabolism, Factor XI Deficiency blood, Factor XI Deficiency drug therapy, Factor XI Deficiency metabolism, Factor XII metabolism, Factor XII Deficiency blood, Factor XII Deficiency drug therapy, Factor XII Deficiency metabolism, Hemostasis drug effects, Hemostasis physiology, Humans, Anticoagulants pharmacology, Factor XI antagonists & inhibitors, Factor XII antagonists & inhibitors, Thrombosis drug therapy, Thrombosis metabolism

Abstract

Purpose of Review: Arterial and venous thrombosis are major causes of morbidity and mortality, and the incidence of thromboembolic diseases increases as a population ages. Thrombi are formed by activated platelets and fibrin. The latter is a product of the plasma coagulation system. Currently available anticoagulants such as heparins, vitamin K antagonists and inhibitors of thrombin or factor Xa target enzymes of the coagulation cascade that are critical for fibrin formation. However, fibrin is also necessary for terminating blood loss at sites of vascular injury. As a result, anticoagulants currently in clinical use increase the risk of bleeding, partially offsetting the benefits of reduced thrombosis. This review focuses on new targets for anticoagulation that are associated with minimal or no therapy-associated increased bleeding., Recent Findings: Data from experimental models using mice and clinical studies of patients with hereditary deficiencies of coagulation factors XI or XII have shown that both of these clotting factors are important for thrombosis, while having minor or no apparent roles in processes that terminate blood loss (hemostasis)., Summary: Hereditary deficiency of factor XII (Hageman factor) or factor XI, plasma proteases that initiate the intrinsic pathway of coagulation, impairs thrombus formation and provides protection from vascular occlusive events, while having a minimal impact on hemostasis. As the factor XII-factor XI pathway contributes to thrombus formation to a greater extent than to normal hemostasis, pharmacological inhibition of these coagulation factors may offer the exciting possibility of anticoagulation therapies with minimal or no bleeding risk.

Published

2011

6. Factor XII: what does it contribute to our understanding of the physiology and pathophysiology of hemostasis & thrombosis.

Author

Stavrou E and Schmaier AH

Subjects

Animals, Blood Coagulation physiology, Factor XII Deficiency metabolism, Mice, Factor XII physiology, Hemostasis physiology, Thrombosis metabolism

Abstract

Factor XII (FXII) is a coagulation protein that is essential for surface-activated blood coagulation tests but whose deficiency is not associated with bleeding. For over forty years, investigators in hemostasis have not considered FXII important because its deficiency is not associated with bleeding. It is because there is a dichotomy between abnormal laboratory assay findings due to FXII deficiency and clinical hemostasis that investigators sought explanations for physiologic hemostasis independent of FXII. FXII is a multidomain protein that contains two fibronectin binding consensual sequences, two epidermal growth factor regions, a kringle region, a proline-rich domain, and a catalytic domain that when proteolyzed turns into a plasma serine protease. Recent investigations with FXII deleted mice that are protected from thrombosis indicate that it contributes to the extent of developing thrombus in the intravascular compartment. These findings suggest that it has a role in thrombus formation without influencing hemostasis. Last, FXII has been newly appreciated to be a growth factor that may influence tissue injury repair and angiogenesis. These combined studies suggest that FXII may become a pharmacologic target to reduce arterial thrombosis risk and promote cell repair after injury, without influencing hemostasis., ((c) 2009 Elsevier Ltd. All rights reserved.)

Published

2010

7. Plasma levels of bradykinin are suppressed in factor XII-deficient mice.

Author

Iwaki T and Castellino FJ

Subjects

Animals, Blood Coagulation, Bradykinin analysis, Enzyme-Linked Immunosorbent Assay methods, Factor XI genetics, Factor XI metabolism, Factor XII metabolism, Factor XII Deficiency genetics, Factor XII Deficiency metabolism, Filtration, Gene Expression Regulation, Kininogen, High-Molecular-Weight genetics, Kininogen, High-Molecular-Weight metabolism, Membranes, Artificial, Mice, Mice, Knockout, Partial Thromboplastin Time, Prekallikrein genetics, Prekallikrein metabolism, RNA, Messenger metabolism, Radioimmunoassay methods, Tissue Distribution, Bradykinin blood, Disease Models, Animal, Factor XII genetics, Factor XII Deficiency blood, Mice, Inbred C57BL

Abstract

A genetically-transmissible factor (F) XII-inactivated allele has been produced in mice by targeted replacement of exons 3-8 of the FXII gene with the neomycin resistance gene. Interbreeding of these mice provided offspring homozygous for two inactivated FXII alleles (FXII(-/-)). Male and female FXII-deficient mice bred normally in all genotypic combinations of the heterozygous and homozygous states, and the offspring survived to adulthood, suggesting that a total FXII deficiency does not affect embryonic development and survival. Neither FXII transcripts nor FXII antigen was found in various tissues of adult FXII(-/-) mice. No obvious unchallenged coagulopathies were present in FXII(-/-) adult mice, despite greatly prolonged activated partial thromboplastin times in this mouse cohort. FXII(-/-) mice were then used to assess the in vivo importance of the plasma FXII/prekallikrein/kininogen pathway in provision of resting plasma bradykinin (BK) levels and in generation of plasma BK stimulated by contact with an artificial surface, using a new and greatly improved plasma BK assay developed during these studies. It was found that approximately 50% of resting BK, and all of the contact-stimulated plasma BK, was provided by this FXII-dependent pathway, without a requirement for FXI. These results provide clear evidence that surface-stimulated BK production, in mice, is dependent on the activation of FXII.

Published

2006

8. Are hemostasis and thrombosis two sides of the same coin?

Author

Colman RW

Subjects

Animals, Blood Coagulation Factor Inhibitors administration & dosage, Blood Vessels metabolism, Blood Vessels pathology, Brain Ischemia drug therapy, Brain Ischemia pathology, Factor XI Deficiency drug therapy, Factor XI Deficiency metabolism, Factor XI Deficiency pathology, Factor XII antagonists & inhibitors, Factor XII metabolism, Factor XII Deficiency pathology, Female, Fibrin metabolism, Male, Mice, Mice, Knockout, Thrombosis drug therapy, Thrombosis pathology, Brain Ischemia metabolism, Factor XII Deficiency metabolism, Hemostasis drug effects, Thrombosis metabolism

Abstract

Factor XII (FXII), a clotting enzyme that can initiate coagulation in vitro, has long been considered dispensable for normal blood clotting in vivo because hereditary deficiencies in FXII are not associated with spontaneous or excessive bleeding. However, new studies show that mice lacking FXII are protected against arterial thrombosis (obstructive clot formation) and stroke. Thus, FXII could be a unique drug target that could be blocked to prevent thrombosis without the side effect of increased bleeding.

Published

2006

9. Targeting coagulation factor XII provides protection from pathological thrombosis in cerebral ischemia without interfering with hemostasis.

Author

Kleinschnitz C, Stoll G, Bendszus M, Schuh K, Pauer HU, Burfeind P, Renné C, Gailani D, Nieswandt B, and Renné T

Subjects

Animals, Blood Coagulation Factor Inhibitors administration & dosage, Blood Vessels metabolism, Blood Vessels pathology, Brain Ischemia pathology, Brain Ischemia prevention & control, Factor XI Deficiency drug therapy, Factor XI Deficiency metabolism, Factor XI Deficiency pathology, Factor XII antagonists & inhibitors, Factor XII Deficiency pathology, Female, Fibrin metabolism, Male, Mice, Mice, Knockout, Thrombosis drug therapy, Thrombosis pathology, Brain Ischemia metabolism, Factor XII metabolism, Factor XII Deficiency metabolism, Hemostasis drug effects, Thrombosis metabolism

Abstract

Formation of fibrin is critical for limiting blood loss at a site of blood vessel injury (hemostasis), but may also contribute to vascular thrombosis. Hereditary deficiency of factor XII (FXII), the protease that triggers the intrinsic pathway of coagulation in vitro, is not associated with spontaneous or excessive injury-related bleeding, indicating FXII is not required for hemostasis. We demonstrate that deficiency or inhibition of FXII protects mice from ischemic brain injury. After transient middle cerebral artery occlusion, the volume of infarcted brain in FXII-deficient and FXII inhibitor-treated mice was substantially less than in wild-type controls, without an increase in infarct-associated hemorrhage. Targeting FXII reduced fibrin formation in ischemic vessels, and reconstitution of FXII-deficient mice with human FXII restored fibrin deposition. Mice deficient in the FXII substrate factor XI were similarly protected from vessel-occluding fibrin formation, suggesting that FXII contributes to pathologic clotting through the intrinsic pathway. These data demonstrate that some processes involved in pathologic thrombus formation are distinct from those required for normal hemostasis. As FXII appears to be instrumental in pathologic fibrin formation but dispensable for hemostasis, FXII inhibition may offer a selective and safe strategy for preventing stroke and other thromboembolic diseases.

Published

2006

10. Phenotypic consequences of genetic variation at hemizygous alleles: Sotos syndrome is a contiguous gene syndrome incorporating coagulation factor twelve (FXII) deficiency.

Author

Kurotaki N, Shen JJ, Touyama M, Kondoh T, Visser R, Ozaki T, Nishimoto J, Shiihara T, Uetake K, Makita Y, Harada N, Raskin S, Brown CW, Höglund P, Okamoto N, and Lupski JR

Subjects

Adolescent, Adult, Child, Child, Preschool, Chromosome Deletion, Factor XII genetics, Factor XII metabolism, Factor XII Deficiency metabolism, Factor XII Deficiency physiopathology, Female, Genetic Variation, Histone Methyltransferases, Histone-Lysine N-Methyltransferase, Humans, In Situ Hybridization, Infant, Intracellular Signaling Peptides and Proteins genetics, Male, Nuclear Proteins genetics, Point Mutation, Syndrome, Factor XII Deficiency genetics, Phenotype

Abstract

Purpose: We tested the hypothesis that Sotos syndrome (SoS) due to the common deletion is a contiguous gene syndrome incorporating plasma coagulation factor twelve (FXII) deficiency. The relationship between FXII activity and the genotype at a functional polymorphism of the FXII gene was investigated., Methods: A total of 21 patients including those with the common deletion, smaller deletions, and point mutations, and four control individuals were analyzed. We examined FXII activity in patients and controls, and analyzed their FXII 46C/T genotype using direct DNA sequencing., Results: Among 10 common deletion patients, seven patients had lower FXII activity with the 46T allele of the FXII gene, whereas three patients had normal FXII activity with the 46C allele. Two patients with smaller deletions, whose FXII gene is not deleted had low FXII activity, but one patient with a smaller deletion had normal FXII. Four point mutation patients and controls all had FXII activities within the normal range., Conclusion: FXII activity in SoS patients with the common deletion is predominantly determined by the functional polymorphism of the remaining hemizygous FXII allele. Thus, Sotos syndrome is a contiguous gene syndrome incorporating coagulation factor twelve (FXII) deficiency.

Published

2005

11. Defective thrombus formation in mice lacking coagulation factor XII.

Author

Renné T, Pozgajová M, Grüner S, Schuh K, Pauer HU, Burfeind P, Gailani D, and Nieswandt B

Subjects

Animals, Collagen administration & dosage, Epinephrine administration & dosage, Factor VIIa metabolism, Factor XII Deficiency genetics, Factor XIIa genetics, Hemorrhage genetics, Hemorrhage metabolism, Lung metabolism, Lung pathology, Mice, Mice, Mutant Strains, Platelet Aggregation drug effects, Platelet Aggregation genetics, Thromboembolism chemically induced, Thromboembolism drug therapy, Thromboembolism pathology, Vasoconstrictor Agents administration & dosage, Blood Coagulation drug effects, Blood Coagulation genetics, Factor XII Deficiency metabolism, Factor XIIa metabolism, Thromboembolism metabolism

Abstract

Blood coagulation is thought to be initiated by plasma protease factor VIIa in complex with the membrane protein tissue factor. In contrast, coagulation factor XII (FXII)-mediated fibrin formation is not believed to play an important role for coagulation in vivo. We used FXII-deficient mice to study the contributions of FXII to thrombus formation in vivo. Intravital fluorescence microscopy and blood flow measurements in three distinct arterial beds revealed a severe defect in the formation and stabilization of platelet-rich occlusive thrombi. Although FXII-deficient mice do not experience spontaneous or excessive injury-related bleeding, they are protected against collagen- and epinephrine-induced thromboembolism. Infusion of human FXII into FXII-null mice restored injury-induced thrombus formation. These unexpected findings change the long-standing concept that the FXII-induced intrinsic coagulation pathway is not important for clotting in vivo. The results establish FXII as essential for thrombus formation, and identify FXII as a novel target for antithrombotic therapy.

Published

2005

12. Recurrent abortion-antibodies to factor XII or a decrease in factor XII levels?

Author

Jones DW, Gallimore MJ, and Winter M

Subjects

Abortion, Habitual immunology, Factor XII immunology, Factor XII metabolism, Female, Humans, Immunoglobulin Allotypes genetics, Immunoglobulin Allotypes physiology, Placenta physiology, Pregnancy, Abortion, Habitual metabolism, Factor XII Deficiency metabolism

Published

2001

13. Factor XII Tenri, a novel cross-reacting material negative factor XII deficiency, occurs through a proteasome-mediated degradation.

Author

Kondo S, Tokunaga F, Kawano S, Oono Y, Kumagai S, and Koide T

Subjects

Adult, Base Sequence, Consanguinity, DNA Mutational Analysis, Deoxyribonucleases, Type II Site-Specific metabolism, Factor XII Deficiency metabolism, Glycoproteins metabolism, Humans, Male, Mutagenesis, Site-Directed, Pedigree, Polymerase Chain Reaction, Polymorphism, Single-Stranded Conformational, Proteasome Endopeptidase Complex, Sequence Analysis, DNA, Cysteine Endopeptidases metabolism, Factor XII metabolism, Factor XII Deficiency genetics, Membrane Glycoproteins, Multienzyme Complexes metabolism, Mutation, Trypsin Inhibitor, Kunitz Soybean

Abstract

A homozygous cross-reacting material negative factor XII-deficient patient with 3% antigen and activity levels of factor XII was screened for the identification of a mutation at the genomic level. Low-ionic strength single-stranded conformation polymorphism (SSCP) analysis and sequence analysis showed that the proband's gene for factor XII had an A-->G substitution at nucleotide position 7832 in exon 3, resulting in a Tyr34 to Cys substitution in the NH2-terminal type II domain of factor XII. We designated this mutation as factor XII Tenri. Mutagenic polymerase chain reaction (PCR), followed by KpnI digestion, showed a homozygous mutation in the proband's gene and heterozygous mutations in his parents and sister. Immunoprecipitation and Western blot analyses of plasma samples from the factor XII Tenri family indicated that the proband had a trace amount of variant factor XII with an apparent molecular mass of 115 kD, which was converted to the normal 80-kD form after reduction, suggesting that factor XII Tenri was secreted as a disulfide-linked heterodimer with a approximately 35-kD protein, which we identified as alpha1-microglobulin by immunoblotting. Pulse-chase experiments using baby hamster kidney (BHK) cells showed that Tenri-type factor XII was extensively degraded intracellularly, but the addition of cystine resulted in increased secretion of the mutant. Using membrane-permeable inhibitors, we observed that the degradation occurred in the pre-Golgi, nonlysosomal compartment and a proteasome appeared to play a major role in this process. On the basis of these in vitro results, we speculate that the majority of the factor XII Tenri is degraded intracellularly through a quality control mechanism in the endoplasmic reticulum (ER), and a small amount of factor XII Tenri that formed a disulfide-linked heterodimer with alpha1-microglobulin is secreted into the blood stream.

Published

1999

14. Transient lupus anticoagulant associated with hypoprothrombinemia and factor XII deficiency following adenovirus infection.

Author

Jaeger U, Kapiotis S, Pabinger I, Puchhammer E, Kyrle PA, and Lechner K

Subjects

Adenoviridae Infections complications, Antibodies analysis, Cardiolipins immunology, Child, Child, Preschool, Factor XII Deficiency complications, Feces microbiology, Female, Humans, Hypoprothrombinemias complications, Male, Adenoviridae Infections metabolism, Factor XII Deficiency metabolism, Hypoprothrombinemias metabolism, Lupus Coagulation Inhibitor metabolism

Abstract

A potent lupus anticoagulant (LA) was detected in four children, 1 week after the clinical onset of an adenovirus infection. The adenovirus infection was documented by direct virus detection in the stool of one patient and serologically in the others. None of the children had elevated titers of IgM- and only one of IgG-anticardiolipin antibodies (ACA). All patients had a marked reduction of prothrombin activity as well as antigen. Prothrombin-antibody complexes were demonstrated in the patients' plasma or mixtures of patient and normal plasma. Factor XII activity was moderately reduced in three of the patients. All coagulation abnormalities returned to normal within 4-12 weeks. Localized bleeding was observed in two cases, but there was no generalized bleeding tendency or evidence of thrombosis.

Published

1993

15. Activation of human plasma prekallikrein by Pseudomonas aeruginosa elastase in vitro.

Author

Shibuya Y, Tanaka H, Nishino N, Okabe H, Kambara T, and Yamamoto T

Subjects

Amino Acid Sequence, Enzyme Activation, Factor XII Deficiency metabolism, Kinetics, Molecular Sequence Data, Pancreatic Elastase antagonists & inhibitors, Pancreatic Elastase metabolism, Prekallikrein metabolism, Pseudomonas aeruginosa enzymology

Abstract

Human plasma prekallikrein, precursor of the bradykinin-generating enzyme, was activated in a purified system under a near physiological condition (pH 7.8, ionic strength I = 0.14, 37 degrees C) by Pseudomonas aeruginosa elastase which is a tissue-destructive metalloproteinase. Compared with that, Pseudomonas aeruginosa alkaline proteinase poorly activated it with a rate as low as less than one-twentieth of that of elastase. The activation by elastase was blocked with a specific inhibitor of elastase, HONHCOCH(CH2C6H5)CO-Ala-Gly-NH2 (10 microM). Generation of kallikrein-like amidolytic activity was also observed in plasma deficient in Hageman factor by treatment with elastase, but was not in plasma deficient in prekallikrein. The kallikrein-like activity generated in Hageman factor deficient plasma as well as the generation process itself was indeed inhibited by anti-human prekallikrein goat antibody. These results suggest that the pathological activation of the kallikrein-kinin system might occur under certain clinical conditions in pseudomonal infections.

Published

1991

16. Abnormal proteolytic degradation of von Willebrand factor after desmopressin infusion in a new subtype of von Willebrand disease (ID).

Author

Lopez-Fernandez MF, Gonzalez-Boullosa R, Blanco-Lopez MJ, Perez M, and Batlle J

Subjects

Adult, Child, Preschool, Deamino Arginine Vasopressin administration & dosage, Electrophoresis, Agar Gel, Factor XII Deficiency genetics, Factor XII Deficiency metabolism, Factor XII Deficiency pathology, Humans, Infusions, Intravenous, Male, Peptide Fragments analysis, Peptide Fragments metabolism, von Willebrand Diseases classification, von Willebrand Diseases genetics, von Willebrand Factor analysis, Deamino Arginine Vasopressin pharmacology, von Willebrand Diseases metabolism, von Willebrand Factor metabolism

Abstract

We describe two members of a single family, father and son, with mild factor XII deficiency associated to von Willebrand disease (vWD) with aberrant structure in whom distinct multimeric abnormalities and an abnormal proteolytic processing of von Willebrand factor (vWF) after desmopressin (DDAVP) administration were present. They had a mild bleeding history, low levels of vWF-related activities, and a prolonged bleeding time. Low-resolution agarose gel electrophoresis showed a vWF with all size multimers in plasma and platelets. Higher-resolution agarose gels demonstrated that the main band was present, but the relative proportion of the satellite bands was markedly reduced. The smallest oligomer was not increased. After the infusion of DDAVP to the father, a transient increase in the relative proportion of the satellite bands was seen, as described in normal individuals. No difference in the structure of vWF was observed when blood was collected with proteinase inhibitors. The analysis of native subunits of vWF and their proteolytic derived fragments, after DDAVP administration, showed a temporary augmentation of the 176 kDa fragment, as seen in normal subjects, as well as an increase of the 189 kDa fragment. This finding had not been reported previously either in normal individuals or in patients with vWD.

Published

1991

17. Contact activation of human plasma prorenin in vitro.

Author

Blumberg AL, Sealey JE, Atlas SA, Laragh JH, Dharmgrongartama B, and Kaplan AP

Subjects

Dialysis, Enzyme Activation, Factor XII Deficiency metabolism, Humans, Hydrogen-Ion Concentration, Kaolin pharmacology, Peptide Hydrolases metabolism, Prekallikrein metabolism, Enzyme Precursors blood, Renin blood

Abstract

Acid activation of plasma prorenin occurs during dialysis to pH 3.3. and also during subsequent dialysis to pH 7.4. The latter, alkaline phase, involves Hageman factor-dependent formation of kallikrein, which in turn activates prorenin. The present study evaluates whether prorenin activation always occurs whenever kallikrein is activated in plasma. TAME esterase activity was used as a measure of plasma kallikrein activity an increase was observed during the alkaline phase of acid activation of prorenin. TAME esterase activity was absent when Hageman factor- or prekallikrein-deficient plasmas were similarly assayed and prorenin was not activated. Kaolin treatment of normal plasma rapidly increased TAME esterase activity at both 25 degrees and -4 degrees C, but no prorenin activation occurred. Similar changes in TAME esterase activity were observed in acid-treated plasma, in which setting prorenin was activated. No change in TAME esterase or renin activity occurred after addition of kaolin to acid-treated plasma deficient in Hageman factor; however, both enzymatic activities increased slightly in acidified prekallikrein-deficient plasma. Mixtures of these deficient plasmas exhibited normal kaolin activation of both TAME esterase and prorenin after acidification. Thus both Hageman factor and prekallikrein are needed for optimal contact activation of prorenin. These results demonstrate that prorenin activation does not always occur when active kallikrein is present in plasma. Prior acidification appears to be a prerequisite. Acidified prorenin may be more susceptible to cleavage; alternatively, competing substrates and/or inhibitors of kallikrein may be destroyed at acid pH, thereby permitting kallikrein to activate prorenin. Under normal conditions, activation of the plasma kallikrein-kinin system appears unlikely to result in activation of prorenin in vivo.

Published

1981

18. Urinary excretion of Hageman factor (factor XII) and the presence of nonfunctional Hageman factor in the nephrotic syndrome.

Author

Saito H, Goodnough LT, Makker SP, and Kallen RJ

Subjects

Adolescent, Centrifugation, Density Gradient, Child, Child, Preschool, Chromatography, Gel, Factor XII Deficiency metabolism, Female, Humans, Male, Nephrotic Syndrome etiology, Prekallikrein deficiency, Radioimmunoassay, Factor XII metabolism, Nephrotic Syndrome metabolism

Abstract

Acquired deficiencies of functional Hageman factor (factor XII) and prekallikrein, proteins involved in the plasma kinin-generating system, have been previously reported in the nephrotic syndrome. The basis for these changes, however, is not fully understood. We have examined the levels of Hageman factor and prekallikrein by functional and radioimmunoassays in plasmas and urines of 11 patients with the nephrotic syndrome. All 11 patients had decreased titers of plasma Hageman factor activity (mean +/- standard deviation (SD), 0.29 +/- 0.15 U/ml), but essentially normal titers of immunoreactive Hageman factor (0.68 +/- 0.23 U/ml). The ratio of immunoreactive Hageman factor to functional Hageman factor (2.63 +/- 0.86) was significantly higher than that in nine control patients (1.08 +/- 0.17). Since no circulating anticoagulants against Hageman factor were detected, these data suggest the presence of nonfunctional (altered) Hageman factor in plasmas of patients with the nephrotic syndrome. Urinary excretion of Hageman factor was present in six patients but did not appear to account for the reduced plasma Hageman factor activity. Urinary Hageman factor in one patient had the same size as plasma Hageman factor as assessed by gel filtration and sucrose density gradient centrifugation. The titers of plasma prekallikrein were within the normal range. These studies indicate urinary excretion of Hageman factor and alterations in the functional sites of plasma Hageman factor molecules in the nephrotic syndrome. Whether these changes are related to the pathogenesis of the nephrotic syndrome remains to be determined.

Published

1981

19. Factor XII-induced fibrinolysis. Diminished proactivator activity and drastic reduction of activator activity in Fletcher factor-deficient plasma gamma globulin.

Author

Espana F, Aznar J, and Estelles A

Subjects

Electrophoresis, Polyacrylamide Gel, Factor XII Deficiency genetics, Humans, Plasminogen Activators metabolism, Prekallikrein genetics, Factor XII Deficiency metabolism, Fibrinolysis, Kallikreins isolation & purification, Prekallikrein isolation & purification, gamma-Globulins analysis

Abstract

Fibrinolytic studies in gamma G fractions of three Fletcher factor-deficient plasmas (functionally deficient in prekallikrein) revealed weak or no factor XII-independent activator activity. Two of the three Fletcher trait patients showed no plasminogen activator activity in clot lysis, fibrin plate, and amidolytic assays. The third patient showed no activator activity as determined by clot lysis and amidolytic assays but gave 10% of the activator activity detected in normal undiluted gamma G fraction in absence of HFf when determined by fibrin plate assay. Normal plasma gamma G fractions showed detectable and significant plasminogen activator activity. These fractions did not contain kallikrein or activated factor XI activities, thus indicating that the activator activity could not be attributed to the presence in these fractions or trace of these activated factors. Furthermore, factor XI-deficient plasma gamma G fraction, which was shown to contain no activated prekallikrein, showed normal plasminogen activator activity. Finally, specific antibodies to prekallikrein were shown not to quench the activity of plasminogen activator present in normal plasma gamma fraction. A double genetic deficiency to explain the absence in Fletcher factor-deficient plasma gamma G fractions of both prekallikrein proactivator and activator activities is not likely. Thus plasma prekallikrein, besides being a known plasminogen proactivator, appears to be required for the expression of a plasminogen activator activity.

Published

1982

20. Fibrinolytic activity of euglobulins precipitated from normal or factor XII-deficient plasma in the presence of saturated and unsaturated fatty acids.

Author

Martin NA, Jenks RL, and Astrup T

Subjects

Dextrans pharmacology, Humans, Lauric Acids pharmacology, Linoleic Acids pharmacology, Myristic Acids pharmacology, Palmitic Acids pharmacology, Stearic Acids pharmacology, Factor XII Deficiency metabolism, Fatty Acids pharmacology, Fatty Acids, Unsaturated pharmacology, Fibrinolysis drug effects, Serum Globulins metabolism

Published

1978