Your search keyword '"Prekallikrein metabolism"' showing total 427 results

1. Factor XII and prekallikrein promote microvascular inflammation and psoriasis in mice.

Author

Zhang Y, Chen Z, Guo J, Wan Q, Zhang Y, Li H, Rao H, Yang J, Xu P, Chen H, and Wang M

Subjects

Animals, Female, Humans, Male, Mice, Aminoquinolines pharmacology, Bradykinin pharmacology, Disease Models, Animal, Imiquimod, Inflammation metabolism, Mice, Inbred C57BL, Mice, Knockout, Microvessels drug effects, Microvessels metabolism, Skin blood supply, Skin metabolism, Skin pathology, Skin drug effects, Factor XII metabolism, Factor XII antagonists & inhibitors, Factor XII genetics, Prekallikrein metabolism, Psoriasis metabolism, Psoriasis chemically induced, Psoriasis pathology

Abstract

Background and Purpose: Psoriasis is an autoimmune inflammatory skin disease, featuring microvascular abnormalities and elevated levels of bradykinin. Contact activation of Factor XII can initiate the plasma kallikrein-kinin cascade, producing inflammation and angioedema. The role of Factor XII in psoriasis is unknown., Experimental Approach: The effects of deficiency of Factor XII or its enzymatic substrate, prekallikrein, were examined in the imiquimod-induced mouse model of psoriasis. Skin microcirculation was assessed using intravital confocal microscopy and laser Doppler flowmeter. A novel antibody blocking Factor XII activation was evaluated for psoriasis prevention., Key Results: Expression of Factor XII was markedly up-regulated in human and mouse psoriatic skin. Genetic deletion of Factor XII or prekallikrein, attenuated imiquimod-induced psoriatic lesions in mice. Psoriatic induction increased skin microvascular blood perfusion, causing vasodilation, hyperpermeability and angiogenesis. It also promoted neutrophil-vascular interaction, inflammatory cytokine release and enhanced Factor XII / prekallikrein enzymatic activity with elevated bradykinin. Factor XII or prekallikrein deficiency ameliorated these microvascular abnormalities and abolished bradykinin increase. Antagonism of bradykinin B 2 receptors reproduced the microvascular protection of Factor XII / prekallikrein deficiency, attenuated psoriatic lesions, and prevented protection by Factor XII / prekallikrein deficiency against psoriasis. Furthermore, treatment of mice with Factor XII antibody alleviated experimentally induced psoriasis and suppressed microvascular inflammation., Conclusion and Implications: Activation of Factor XII promoted psoriasis via prekallikrein-dependent formation of bradykinin, which critically mediated psoriatic microvascular inflammation. Inhibition of contact activation represents a novel therapeutic strategy for psoriasis., (© 2024 British Pharmacological Society.)

Published

2024

2. FXII contact activation products have an inhibitory effect on αFXIIa.

Author

Xu LC and Siedlecki CA

Subjects

Humans, Hydrophobic and Hydrophilic Interactions, Factor XIIa metabolism, Factor XIIa antagonists & inhibitors, Prekallikrein metabolism, Glass chemistry, Blood Coagulation drug effects, Factor XII metabolism, Factor XII antagonists & inhibitors, Silanes chemistry, Surface Properties, Wettability

Abstract

It is accepted that the contact activation complex of the intrinsic pathway of blood coagulation cascade produces active enzymes that lead to plasma coagulation following biomaterial contact. In this study, FXII was activated through contact with hydrophilic glass beads and hydrophobic octadecyltrichlorosilane-modified glass beads from neat buffer solutions. These FXII contact activation products generated from material interaction were found to suppress the procoagulant activity of exogenous αFXIIa, and this inhibition was dependent on surface wettability and the concentration of exogenous αFXIIa. Higher relative inhibition rates were generally observed at low concentrations of αFXIIa (1-2 μg/mL) while both hydrophobic and hydrophilic materials showed similar inhibition levels (~39%) at high concentrations of αFXIIa (20 μg/mL). The presence of prekallikrein in the activation system increased the amount of FXIIa produced during FXII contact activation, and also suppressed the apparent levels of inhibitors on hydrophilic surfaces, while having no effect on apparent levels of inhibitors on hydrophobic surface. The combination of FXII contact activation products and activator surfaces was found to dramatically increase inhibition of αFXIIa activity compared to the activation products alone, regardless of activator surface wettability and the presence of prekallikrein. This finding of inhibitors in the suite of proteins generated by contact activation provides additional knowledge into the complex series of interactions that occur when plasma comes into contact with material surfaces., (© 2023 The Authors. Journal of Biomedical Materials Research Part A published by Wiley Periodicals LLC.)

Published

2024

3. Increased Prolylcarboxypeptidase Expression Can Serve as a Biomarker of Senescence in Culture.

Author

Boullard NG, Paris JJ, Shariat-Madar Z, and Mahdi F

Subjects

Humans, Prekallikrein metabolism, Prekallikrein genetics, Bradykinin pharmacology, Bradykinin metabolism, Pulmonary Artery metabolism, Pulmonary Artery cytology, Cells, Cultured, Kininogen, High-Molecular-Weight metabolism, Signal Transduction, Nitric Oxide Synthase Type III metabolism, Nitric Oxide Synthase Type III genetics, Kallikreins metabolism, Kallikreins genetics, Cellular Senescence, Endothelial Cells metabolism, Biomarkers metabolism, Carboxypeptidases metabolism, Carboxypeptidases genetics

Abstract

Prolylcarboxypeptidase (PRCP, PCP, Lysosomal Pro-X-carboxypeptidase, Angiotensinase C) controls angiotensin- and kinin-induced cell signaling. Elevation of PRCP appears to be activated in chronic inflammatory diseases [cardiovascular disease (CVD), diabetes] in proportion to severity. Vascular endothelial cell senescence and mitochondrial dysfunction have consistently been shown in models of CVD in aging. Cellular senescence, a driver of age-related dysfunction, can differentially alter the expression of lysosomal enzymes due to lysosomal membrane permeability. There is a lack of data demonstrating the effect of age-related dysfunction on the expression and function of PRCP. To explore the changes in PRCP, the PRCP-dependent prekallikrein (PK) pathway was characterized in early- and late-passage human pulmonary artery endothelial cells (HPAECs). Detailed kinetic analysis of cells treated with high molecular weight kininogen (HK), a precursor of bradykinin (BK), and PK revealed a mechanism by which senescent HPAECs activate the generation of kallikrein upon the assembly of the HK-PK complex on HPAECs in parallel with an upregulation of PRCP and endothelial nitric oxide (NO) synthase (eNOS) and NO formation. The NO production and expression of both PRCP and eNOS increased in early-passage HPAECs and decreased in late-passage HPAECs. Low activity of PRCP in late-passage HPAECs was associated with rapid decreased telomerase reverse transcriptase mRNA levels. We also found that, with an increase in the passage number of HPAECs, reduced PRCP altered the respiration rate. These results indicated that aging dysregulates PRCP protein expression, and further studies will shed light into the complexity of the PRCP-dependent signaling pathway in aging.

Published

2024

4. Thrombin activation of the factor XI dimer is a multistaged process for each subunit.

Author

Bar Barroeta A, Albanese P, Kadavá T, Jankevics A, Marquart JA, Meijers JCM, and Scheltema RA

Subjects

Humans, Binding Sites, Protein Multimerization, Mutation, Protein Conformation, Blood Coagulation, Prekallikrein metabolism, Prekallikrein chemistry, Protein Subunits metabolism, Enzyme Activation, Factor XIa metabolism, Factor XIa chemistry, Thrombin metabolism, Thrombin chemistry, Factor XI metabolism, Factor XI chemistry, Molecular Dynamics Simulation, Protein Binding

Abstract

Background: Factor (F)XI can be activated by proteases, including thrombin and FXIIa. The interactions of these enzymes with FXI are transient in nature and therefore difficult to study., Objectives: To identify the binding interface between thrombin and FXI and understand the dynamics underlying FXI activation., Methods: Crosslinking mass spectrometry was used to localize the binding interface of thrombin on FXI. Molecular dynamics simulations were applied to investigate conformational changes enabling thrombin-mediated FXI activation after binding. The proposed trajectory of activation was examined with nanobody 1C10, which was previously shown to inhibit thrombin-mediated activation of FXI., Results: We identified a binding interface of thrombin located on the light chain of FXI involving residue Pro520. After this initial interaction, FXI undergoes conformational changes driven by binding of thrombin to the apple 1 domain in a secondary step to allow migration toward the FXI cleavage site. The 1C10 binding site on the apple 1 domain supports this proposed trajectory of thrombin. We validated the results with known mutation sites on FXI. As Pro520 is conserved in prekallikrein (PK), we hypothesized and showed that thrombin can bind PK, even though it cannot activate PK., Conclusion: Our investigations show that the activation of FXI is a multistaged procedure. Thrombin first binds to Pro520 in FXI; thereafter, it migrates toward the activation site by engaging the apple 1 domain. This detailed analysis of the interaction between thrombin and FXI paves a way for future interventions for bleeding or thrombosis., Competing Interests: Declaration of competing interests There are no competing interests to disclose., (Copyright © 2024 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2024

5. High molecular weight kininogen interactions with the homologs prekallikrein and factor XI: importance to surface-induced coagulation.

Author

Mohammed BM, Sun MF, Cheng Q, Litvak M, McCrae KR, Emsley J, McCarty OJT, and Gailani D

Subjects

Animals, Humans, Mice, Factor XI metabolism, Prekallikrein metabolism, Blood Coagulation, Kininogen, High-Molecular-Weight metabolism, Thrombosis

Abstract

Background: In plasma, high molecular weight kininogen (HK) is either free or bound to prekallikrein (PK) or factor (F) XI (FXI). During contact activation, HK is thought to anchor PK and FXI to surfaces, facilitating their conversion to the proteases plasma kallikrein and FXIa. Mice lacking HK have normal hemostasis but are resistant to injury-induced arterial thrombosis., Objectives: To identify amino acids on the HK-D6 domain involved in PK and FXI binding and study the importance of the HK-PK and HK-FXI interactions to coagulation., Methods: Twenty-four HK variants with alanine replacements spanning residues 542-613 were tested in PK/FXI binding and activated partial thromboplastin time clotting assays. Surface-induced FXI and PK activation in plasma were studied in the presence or absence of HK. Kng1 -/- mice lacking HK were supplemented with human or murine HK and tested in an arterial thrombosis model., Results: Overlapping binding sites for PK and FXI were identified in the HK-D6 domain. HK variants with defects only in FXI binding corrected the activated partial thromboplastin time of HK-deficient plasma poorly compared to a variant defective only in PK-binding. In plasma, HK deficiency appeared to have a greater deleterious effect on FXI activation than PK activation. Human HK corrected the defect in arterial thrombus formation in HK-deficient mice poorly due to a specific defect in binding to mouse FXI., Conclusion: Clinical observations indicate FXI is required for hemostasis, while HK is not. Yet, the HK-FXI interaction is required for contact activation-induced clotting in vitro and in vivo suggesting an important role in thrombosis and perhaps other FXI-related activities., Competing Interests: Declaration of competing interests D.G. is a consultant for pharmaceutical companies (Anthos Therapeutics; Aronora, Inc.; Bayer Pharma; Bristol-Myers Squibb; Ionis Pharmaceuticals; Janssen, Pharmaceuticals) with interests in targeting FXI, FXII, and prekallikrein for therapeutic purposes. The other authors have no conflicts to report., (Copyright © 2023 International Society on Thrombosis and Haemostasis. Published by Elsevier Inc. All rights reserved.)

Published

2024

6. Structures of factor XI and prekallikrein bound to domain 6 of high-molecular weight kininogen reveal alternate domain 6 conformations and exosites.

Author

Li C, Barroeta AB, Wong SS, Kim HJ, Pathak M, Dreveny I, Meijers JCM, and Emsley J

Subjects

Humans, Prekallikrein metabolism, Molecular Weight, Binding Sites, Kininogens chemistry, Peptides chemistry, Kininogen, High-Molecular-Weight metabolism, Factor XI metabolism

Abstract

Background: High-molecular weight kininogen (HK) circulates in plasma as a complex with zymogen prekallikrein (PK). HK is both a substrate and a cofactor for activated plasma kallikrein, and the principal exosite interactions occur between PK N-terminal apple domains and the C-terminal D6 domain of HK., Objectives: To determine the structure of the complex formed between PK apple domains and an HKD6 fragment and compare this with the coagulation factor XI (FXI)-HK complex., Methods: We produced recombinant FXI and PK heavy chains (HCs) spanning all 4 apple domains. We cocrystallized PKHC (and subsequently FXIHC) with a 31-amino acid synthetic peptide spanning HK residues Ser565-Lys595 and determined the crystal structure. We also analyzed the full-length FXI-HK complex in solution using hydrogen deuterium exchange mass spectrometry., Results: The 2.3Å PKHC-HK peptide crystal structure revealed that the HKD6 sequence WIPDIQ (Trp569-Gln574) binds to the apple 1 domain and HK FNPISDFPDT (Phe582-Thr591) binds to the apple 2 domain with a flexible intervening sequence resulting in a bent double conformation. A second 3.2Å FXIHC-HK peptide crystal structure revealed a similar interaction with the apple 2 domain but an alternate, straightened conformation of the HK peptide where residues LSFN (Leu579-Asn583) interacts with a unique pocket formed between the apple 2 and 3 domains. HDX-MS of full length FXI-HK complex in solution confirmed interactions with both apple 2 and apple 3., Conclusions: The alternate conformations and exosite binding of the HKD6 peptide likely reflects the diverging relationship of HK to the functions of PK and FXI., Competing Interests: Declaration of competing interests There are no competing interests to disclose., (Crown Copyright © 2023. Published by Elsevier Inc. All rights reserved.)

Published

2023

7. A site on factor XII required for productive interactions with polyphosphate.

Author

Shamanaev A, Litvak M, Cheng Q, Ponczek M, Dickeson SK, Smith SA, Morrissey JH, and Gailani D

Subjects

Humans, Animals, Mice, Prekallikrein metabolism, Polyphosphates, HEK293 Cells, Factor XI metabolism, Factor XIIa metabolism, Factor XII metabolism, Thrombosis

Abstract

Background: During plasma contact activation, factor XII (FXII) binds to surfaces through its heavy chain and undergoes conversion to the protease FXIIa. FXIIa activates prekallikrein and factor XI (FXI). Recently, we showed that the FXII first epidermal growth factor-1 (EGF1) domain is required for normal activity when polyphosphate is used as a surface., Objectives: The aim of this study was to identify amino acids in the FXII EGF1 domain required for polyphosphate-dependent FXII functions., Methods: FXII with alanine substitutions for basic residues in the EGF1 domain were expressed in HEK293 fibroblasts. Wild-type FXII (FXII-WT) and FXII containing the EGF1 domain from the related protein Pro-HGFA (FXII-EGF1) were positive and negative controls. Proteins were tested for their capacity to be activated, and to activate prekallikrein and FXI, with or without polyphosphate, and to replace FXII-WT in plasma clotting assays and a mouse thrombosis model., Results: FXII and all FXII variants were activated similarly by kallikrein in the absence of polyphosphate. However, FXII with alanine replacing Lys 73 , Lys 74 , and Lys 76 (FXII-Ala 73,74,76 ) or Lys 76 , His 78 , and Lys 81 (FXII-Ala 76,78,81 ) were activated poorly in the presence of polyphosphate. Both have <5% of normal FXII activity in silica-triggered plasma clotting assays and have reduced binding affinity for polyphosphate. Activated FXIIa-Ala 73,74,76 displayed profound defects in surface-dependent FXI activation in purified and plasma systems. FXIIa-Ala 73,74,76 reconstituted FXII-deficient mice poorly in an arterial thrombosis model., Conclusion: FXII Lys 73 , Lys 74 , Lys 76 , and Lys 81 form a binding site for polyanionic substances such as polyphosphate that is required for surface-dependent FXII function., Competing Interests: Declaration of competing interests D.G. receives consultant fees from pharmaceutical companies with an interest in the inhibition of contact activation and the kallikrein-kinin system for therapeutic purposes. All other authors have no conflicts to report., (Copyright © 2023 International Society on Thrombosis and Haemostasis. Published by Elsevier Inc. All rights reserved.)

Published

2023

8. Titanium is a potent inducer of contact activation: implications for intravascular devices.

Author

Litvak M, Shamanaev A, Zalawadiya S, Matafonov A, Kobrin A, Feener EP, Wallisch M, Tucker EI, McCarty OJT, and Gailani D

Subjects

Humans, Factor XI metabolism, Factor XII metabolism, Titanium, Kaolin, Prekallikrein metabolism

Abstract

Background: Titanium (Ti) and its alloys are widely used in manufacturing medical devices because of their strength and resistance to corrosion. Although Ti compounds are considered compatible with blood, they appear to support plasma contact activation and may be thrombogenic., Objectives: The objective of this study was to compare Ti and titanium nitride (TiN) with known activators of contact activation (kaolin and silica) in plasma-clotting assays and to assess binding and activation of factor XII, (FXII), factor XI (FXI), prekallikrein, and high-molecular-weight kininogen (HK) with Ti/TiN., Methods: Ti-based nanospheres and foils were compared with kaolin, silica, and aluminum in plasma-clotting assays. Binding and activation of FXII, prekallikrein, HK, and FXI to surfaces was assessed with western blots and chromogenic assays., Results: Using equivalent surface amounts, Ti and TiN were comparable with kaolin and superior to silica, for inducing coagulation and FXII autoactivation. Similar to many inducers of contact activation, Ti and TiN are negatively charged; however, their effects on FXII are not neutralized by the polycation polybrene. Antibodies to FXII, prekallikrein, or FXI or coating Ti with poly-L-arginine blocked Ti-induced coagulation. An antibody to FXII reduced FXII and PK binding to Ti, kallikrein generation, and HK cleavage., Conclusion: Titanium compounds induce contact activation with a potency comparable with that of kaolin. Binding of FXII with Ti shares some features with FXII binding to soluble polyanions but may have unique features. Inhibitors targeting FXII or FXI may be useful in mitigating Ti-induced contact activation in patients with titanium-based implants that are exposed to blood., Competing Interests: Declaration of competing interest statement D.G. is a consultant for pharmaceutical companies (Anthos Therapeutics; Aronora, Inc.; Bayer Pharma; Bristol-Myers Squibb; Ionis Pharmaceuticals; Janssen, Pharmaceuticals) with interests in targeting factor XI, factor XII, and prekallikrein for therapeutic purposes. M.W. and E.I.T are employees of Aronora, and they, as well as Oregon Health and Sciences University, may have financial interest in the results of this study. EPF is an employee of KalVista Pharmaceuticals Inc. The other authors have no conflicts to report., (Copyright © 2022 International Society on Thrombosis and Haemostasis. Published by Elsevier Inc. All rights reserved.)

Published

2023

9. Anti-HK antibody inhibits the plasma contact system by blocking prekallikrein and factor XI activation in vivo.

Author

Chen ZL, Singh PK, Horn K, Calvano MR, Kaneki S, McCrae KR, Strickland S, and Norris EH

Subjects

Humans, Animals, Mice, Factor XI metabolism, Bradykinin pharmacology, Bradykinin chemistry, Kininogen, High-Molecular-Weight chemistry, Kininogen, High-Molecular-Weight metabolism, Prekallikrein chemistry, Prekallikrein metabolism, Thrombosis

Abstract

A dysregulated plasma contact system is involved in various pathological conditions, such as hereditary angioedema, Alzheimer disease, and sepsis. We previously showed that the 3E8 anti-high molecular weight kininogen (anti-HK) antibody blocks HK cleavage and bradykinin generation in human plasma ex vivo. Here, we show that 3E8 prevented not only HK cleavage but also factor XI (FXI) and prekallikrein (PK) activation by blocking their binding to HK in mouse plasma in vivo. 3E8 also inhibited contact system-induced bradykinin generation in vivo. Interestingly, FXII activation was also inhibited, likely because of the ability of 3E8 to block the positive feedback activation of FXII by kallikrein (PKa). In human plasma, 3E8 also blocked PK and FXI binding to HK and inhibited both thrombotic (FXI activation) and inflammatory pathways (PK activation and HK cleavage) of the plasma contact system activation ex vivo. Moreover, 3E8 blocked PKa binding to HK and dose-dependently inhibited PKa cleavage of HK. Our results reveal a novel strategy to inhibit contact system activation in vivo, which may provide an effective method to treat human diseases involving contact system dysregulation., (© 2023 by The American Society of Hematology. Licensed under Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International (CC BY-NC-ND 4.0), permitting only noncommercial, nonderivative use with attribution. All other rights reserved.)

Published

2023

10. Glycated albumin modulates the contact system with implications for the kallikrein-kinin and intrinsic coagulation systems.

Author

Hardy LJ, Bohinc D, Bane KL, Heal SL, Hethershaw E, Ali M, Palmer-Dench T, Foster R, Longstaff C, Renné T, Stavrou EX, and Philippou H

Subjects

Humans, Kinins, Factor XIIa metabolism, Kininogen, High-Molecular-Weight metabolism, Prekallikrein metabolism, Albumins, Glycation End Products, Advanced, Kallikreins metabolism, Plasma Kallikrein metabolism

Abstract

Background: Human serum albumin (HSA) is the most abundant plasma protein and is sensitive to glycation in vivo. The chronic hyperglycemic conditions in patients with diabetes mellitus (DM) induce a nonenzymatic Maillard reaction that denatures plasma proteins and forms advanced glycation end products (AGEs). HSA-AGE is a prevalent misfolded protein in patients with DM and is associated with factor XII activation and downstream proinflammatory kallikrein-kinin system activity without any associated procoagulant activity of the intrinsic pathway., Objectives: This study aimed to determine the relevance of HSA-AGE toward diabetic pathophysiology., Methods: The plasma obtained from patients with DM and euglycemic volunteers was probed for activation of FXII, prekallikrein (PK), and cleaved high-molecular-weight kininogen by immunoblotting. Constitutive plasma kallikrein activity was determined via chromogenic assay. Activation and kinetic modulation of FXII, PK, FXI, FIX, and FX via in vitro-generated HSA-AGE were explored using chromogenic assays, plasma-clotting assays, and an in vitro flow model using whole blood., Results: Plasma obtained from patients with DM contained increased plasma AGEs, activated FXIIa, and resultant cleaved cleaved high-molecular-weight kininogen. Elevated constitutive plasma kallikrein enzymatic activity was identified, which positively correlated with glycated hemoglobin levels, representing the first evidence of this phenomenon. HSA-AGE, generated in vitro, triggered FXIIa-dependent PK activation but limited the intrinsic coagulation pathway activation by inhibiting FXIa and FIXa-dependent FX activation in plasma., Conclusion: These data indicate a proinflammatory role of HSA-AGEs in the pathophysiology of DM via FXII and kallikrein-kinin system activation. A procoagulant effect of FXII activation was lost through the inhibition of FXIa and FIXa-dependent FX activation by HSA-AGEs., Competing Interests: Declaration of competing interests There are no competing interests to disclose., (Copyright © 2023 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2023

11. Severe high-molecular-weight kininogen deficiency: clinical characteristics, deficiency-causing KNG1 variants, and estimated prevalence.

Author

Adenaeuer A, Barco S, Trinchero A, Krutmann S, Nazir HF, Ambaglio C, Rocco V, Pancione Y, Tomao L, Ruiz-Sáez A, Echenagucia M, Alesci S, Sollfrank S, Ezigbo ED, Häuser F, Lackner KJ, Lämmle B, and Rossmann H

Subjects

Prevalence, Blood Coagulation Factors, Kininogen, High-Molecular-Weight genetics, Kininogen, High-Molecular-Weight metabolism, Prekallikrein genetics, Prekallikrein metabolism

Abstract

Background: Severe high-molecular-weight kininogen (HK) deficiency is a poorly studied autosomal recessive contact system defect caused by pathogenic, biallelic KNG1 variants., Aim: We performed the first comprehensive analysis of diagnostic, clinical, genetic, and epidemiological aspects of HK deficiency., Methods: We collected clinical information and blood samples from a newly detected HK-deficient individual and from published cases identified by a systematic literature review. Activity and antigen levels of coagulation factors were determined. Genetic analyses of KNG1 and KLKB1 were performed by Sanger sequencing. The frequency of HK deficiency was estimated considering truncating KNG1 variants from GnomAD., Results: We identified 48 cases of severe HK deficiency (41 families), of these 47 have been previously published (n = 19 from gray literature). We genotyped 3 cases and critically appraised 10 studies with genetic data. Ten HK deficiency-causing variants (one new) were identified. All of them were truncating mutations, whereas the only known HK amino acid substitution with a relevant phenotype instead causes hereditary angioedema. Conservative estimates suggest an overall prevalence of severe HK deficiency of approximately one case per 8 million population, slightly higher in Africans. Individuals with HK deficiency appeared asymptomatic and had decreased levels of prekallikrein and factor XI, which could lead to misdiagnosis., Conclusion: HK deficiency is a rare condition with only few known pathogenic variants. It has an apparently good prognosis but is prone to misdiagnosis. Our understanding of its clinical implications is still limited, and an international prekallikrein and HK deficiency registry is being established to fill this knowledge gap., (Copyright © 2022 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2023

12. In vitro reconstitution of kallikrein-kinin system and progress curve analysis.

Author

Favier B, Bicout DJ, Baroso R, Paclet MH, and Drouet C

Subjects

Humans, Prekallikrein metabolism, Factor XII metabolism, Bradykinin metabolism, Dextran Sulfate, Ice, Reproducibility of Results, Enzyme Precursors metabolism, Serine metabolism, Kallikrein-Kinin System, Kininogen, High-Molecular-Weight metabolism

Abstract

Human kallikrein-kinin system (KKS) is a proteolytic cascade with two serine-protease zymogen couples (Factor XII and prekallikrein (PK) and their activated forms, FXIIa, PKa, respectively), releasing bradykinin by cleavage of native high-molecular-weight kininogen (nHK) into cleaved HK. For KKS investigation in human plasma, this cascade is usually triggered on ice eventually by mixing with purified proteins. It has been established that purified FXIIa, PK, and nHK required a fixed order and timing for mixing protein on ice to ensure reproducibility of testing, we investigated the activation kinetics of both enzymes. The activation process of this in vitro minimal reconstitution of KKS was studied by progress curve analysis, in condition of high enzyme/substrate ratio and by using on natural rather than peptide substrates. FXIIa and PKa were found five-times less active on ice than at 37°C: kcat = 0.133 ± 0.034 and 0.0119 ± 0.0027 s-1, KM = 672 ± 150 and 115 ± 24 nM, respectively. The progress curve analysis of our in vitro KKS reconstitutions differed from a Michaelis-Menten mathematical simulation by a faster initial rate and a slower late rate. These two features were also observed ex vivo by using dextran sulfate-activated plasma and could reinforce the hypothesis of a maximal local effect (bradykinin release) and a minimal systemic consequence (PK preservation) in KKS activation process. Analyzing the complete curve of cold KKS activation would provide valuable information for ex vivo investigation of KKS in samples from patients presenting with hereditary angioedema and other inflammatory conditions., (© 2022 The Author(s).)

Published

2022

13. Pharmacological suppression of the kallikrein kinin system with KVD900: An orally available plasma kallikrein inhibitor for the on-demand treatment of hereditary angioedema.

Author

Duckworth EJ, Murugesan N, Li L, Rushbrooke LJ, Lee DK, De Donatis GM, Maetzel A, Yea CM, Hampton SL, and Feener EP

Subjects

Bradykinin, Complement C1 Inhibitor Protein genetics, Factor XII, Fluorescent Dyes therapeutic use, Humans, Kallikrein-Kinin System, Plasma Kallikrein, Prekallikrein metabolism, Angioedemas, Hereditary drug therapy, Angioedemas, Hereditary prevention & control

Abstract

Background: Hereditary angioedema (HAE) is a rare genetic disease that leads to recurrent episodes of swelling and pain caused by uncontrolled plasma kallikrein (PKa) activity. Current guidelines recommend ready availability of on-demand HAE treatments that can be administered early upon attack onset. This report describes the pharmacological and pharmacodynamic properties of the novel oral small-molecule PKa inhibitor KVD900 as a potential on-demand treatment for HAE., Methods: Pharmacological properties of KVD900 on PKa and closely related serine proteases were characterized using kinetic fluorogenic substrate activity assays. Effects of KVD900 on PKa activity and kallikrein kinin system activation in whole plasma were measured in the presence of dextran sulphate (DXS)-stimulation using a fluorogenic substrate and capillary immunoassays to quantify high molecular weight kininogen (HK), plasma prekallikrein and Factor XII cleavage. Pharmacodynamic effects of orally administered KVD900 were characterized in plasma samples from six healthy controls in a first in human phase 1 clinical trial and from 12 participants with HAE in a phase 2 clinical trial., Results: KVD900 is a selective, competitive and reversible inhibitor of human PKa enzyme with a K i of 3.02 nM. The association constant (K on ) of KVD900 for PKa is >10 × 10 6  M -1  s -1 . Oral administration of KVD900 in a first-in-human clinical trial achieved rapid and near complete inhibition of DXS-stimulated PKa enzyme activity and HK cleavage and reduced plasma prekallikrein and Factor XII activation in plasma. In individuals with HAE, orally administered KVD900 inhibited DXS-stimulated PKa activity in plasma by ≥95% from 45 min to at least 4 h post-dose and provided rapid protection of HK from cleavage., Conclusion: KVD900 is a fast-acting oral PKa inhibitor that rapidly inhibits PKa activity, kallikrein kinin system activation and HK cleavage in plasma. On-demand administration of KVD900 may provide an opportunity to halt the generation of bradykinin and reverse HAE attacks., (© 2022 KalVista Pharmaceuticals, Inc. Clinical & Experimental Allergy published by John Wiley & Sons Ltd.)

Published

2022

14. Recent advances in factor XII structure and function.

Author

Shamanaev A, Litvak M, and Gailani D

Subjects

Blood Coagulation, Fibronectins, Humans, Kallikreins, Factor XII metabolism, Prekallikrein metabolism

Abstract

Purpose of Review: Factor XII (FXII), the precursor of the protease FXIIa, contributes to pathologic processes including angioedema and thrombosis. Here, we review recent work on structure-function relationships for FXII based on studies using recombinant FXII variants., Recent Findings: FXII is a homolog of pro-hepatocyte growth factor activator (Pro-HGFA). We prepared FXII in which domains are replaced by corresponding parts of Pro-HGA, and tested them in FXII activation and activity assays. In solution, FXII and prekallikrein undergo reciprocal activation to FXIIa and kallikrein. The rate of this process is restricted by the FXII fibronectin type-2 and kringle domains. Pro-HGA replacements for these domains accelerate FXII and prekallikrein activation. When FXII and prekallikrein bind to negatively charged surfaces, reciprocal activation is enhanced. The FXII EGF1 domain is required for surface binding., Summary: We propose a model in which FXII is normally maintained in a closed conformation resistant to activation by intramolecular interactions involving the fibronectin type-2 and kringle domains. These interactions are disrupted when FXII binds to a surface through EGF1, enhancing FXII activation and prekallikrein activation by FXIIa. These observations have important implications for understanding the contributions of FXII to disease, and for developing therapies to treat thrombo-inflammatory disorders., (Copyright © 2022 Wolters Kluwer Health, Inc. All rights reserved.)

Published

2022

15. Anti-HK antibody reveals critical roles of a 20-residue HK region for Aβ-induced plasma contact system activation.

Author

Chen ZL, Singh PK, Horn K, Strickland S, and Norris EH

Subjects

Amino Acids, Antibodies, Factor XI metabolism, Factor XII, Humans, Prekallikrein metabolism, Alzheimer Disease, Kininogen, High-Molecular-Weight metabolism

Abstract

Alzheimer's disease (AD) is a neurodegenerative disorder and the leading cause of dementia. Vascular abnormalities and neuroinflammation play roles in AD pathogenesis. Plasma contact activation, which leads to fibrin clot formation and bradykinin release, is elevated in many AD patients, likely due to the ability of AD's pathogenic peptide β-amyloid (Aβ) to induce its activation. Since overactivation of this system may be deleterious to AD patients, the development of inhibitors could be beneficial. Here, we show that 3E8, an antibody against a 20-amino acid region in domain 6 of high molecular weight kininogen (HK), inhibits Aβ-induced intrinsic coagulation. Mechanistically, 3E8 inhibits contact system activation by blocking the binding of prekallikrein (PK) and factor XI (FXI) to HK, thereby preventing their activation and the continued activation of factor XII (FXII). The 3E8 antibody can also disassemble HK/PK and HK/FXI complexes in normal human plasma in the absence of a contact system activator due to its strong binding affinity for HK, indicating its prophylactic ability. Furthermore, the binding of Aβ to both FXII and HK is critical for Aβ-mediated contact system activation. These results suggest that a 20-amino acid region in domain 6 of HK plays a critical role in Aβ-induced contact system activation, and this region may provide an effective strategy to inhibit or prevent contact system activation in related disorders., (© 2022 by The American Society of Hematology. Licensed under Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International (CC BY-NC-ND 4.0), permitting only noncommercial, nonderivative use with attribution. All other rights reserved.)

Published

2022

16. Model for surface-dependent factor XII activation: the roles of factor XII heavy chain domains.

Author

Shamanaev A, Ivanov I, Sun MF, Litvak M, Srivastava P, Mohammed BM, Shaban R, Maddur A, Verhamme IM, McCarty OJT, Law RHP, and Gailani D

Subjects

Aminocaproic Acid, Blood Coagulation, Fibronectins chemistry, Lysine, Factor XII chemistry, Prekallikrein chemistry, Prekallikrein metabolism

Abstract

Factor XII (FXII) is the zymogen of a plasma protease (FXIIa) that contributes to bradykinin generation by converting prekallikrein to the protease plasma kallikrein (PKa). FXII conversion to FXIIa by autocatalysis or PKa-mediated cleavage is enhanced when the protein binds to negatively charged surfaces such as polymeric orthophosphate. FXII is composed of noncatalytic (heavy chain) and catalytic (light chain) regions. The heavy chain promotes FXII surface-binding and surface-dependent activation but restricts activation when FXII is not surface bound. From the N terminus, the heavy chain contains fibronectin type 2 (FN2), epidermal growth factor-1 (EGF1), fibronectin type 1 (FN1), EGF2, and kringle (KNG) domains and a proline-rich region. It shares this organization with its homolog, pro-hepatocyte growth factor activator (Pro-HGFA). To study the importance of heavy chain domains in FXII function, we prepared FXII with replacements of each domain with corresponding Pro-HGFA domains and tested them in activation and activity assays. EGF1 is required for surface-dependent FXII autoactivation and surface-dependent prekallikrein activation by FXIIa. KNG and FN2 are important for limiting FXII activation in the absence of a surface by a process that may require interactions between a lysine/arginine binding site on KNG and basic residues elsewhere on FXII. This interaction is disrupted by the lysine analog ε-aminocaproic acid. A model is proposed in which an ε-aminocaproic acid-sensitive interaction between the KNG and FN2 domains maintains FXII in a conformation that restricts activation. Upon binding to a surface through EGF1, the KNG/FN2-dependent mechanism is inactivated, exposing the FXII activation cleavage site., (© 2022 by The American Society of Hematology. Licensed under Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International (CC BY-NC-ND 4.0), permitting only noncommercial, nonderivative use with attribution. All other rights reserved.)

Published

2022

17. Identification of the histidine-rich glycoprotein domains responsible for contact pathway inhibition.

Author

Truong TK, Malik RA, Yao X, Fredenburgh JC, Stafford AR, Madarati HM, Kretz CA, and Weitz JI

Subjects

Animals, Factor XII metabolism, Factor XIIa metabolism, Humans, Mice, Peptides pharmacology, Polyphosphates, Proteins, Prekallikrein metabolism, Thrombin metabolism

Abstract

Background: Previously, we showed that histidine-rich glycoprotein (HRG) binds factor (F) XIIa with high affinity, inhibits FXII autoactivation and FXIIa-mediated activation of FXI, and attenuates ferric chloride-induced arterial thrombosis in mice. Therefore, HRG downregulates the contact pathway in vitro and in vivo., Objective: To identify the domains on HRG responsible for contact pathway inhibition., Methods: Recombinant HRG domain constructs (N-terminal [N1, N2, and N1N2], proline-rich regions, histidine-rich region [HRR], and C-terminal) were expressed and purified. The affinities of plasma-derived HRG, HRG domain constructs, and synthetic HRR peptides for FXII, FXIIa, β-FXIIa, and polyphosphate (polyP) were determined using surface plasmon resonance, and their effects on polyP-induced FXII autoactivation, FXIIa-mediated activation of FXI and prekallikrein, the activated partial thromboplastin time (APTT), and thrombin generation were examined., Results: HRG and HRG domain constructs bind FXIIa, but not FXII or β-FXII. HRR, N1, and N1N2 bind FXIIa with affinities comparable with that of HRG, whereas the remaining domains bind with lower affinity. Synthetic HRR peptides bind FXIIa and polyP with high affinity. HRG and HRR significantly inhibit FXII autoactivation and prolong the APTT. Like HRG, synthetic HRR peptides inhibit FXII autoactivation, attenuate FXIIa-mediated activation of prekallikrein and FXI, prolong the APTT, and attenuate thrombin generation., Conclusion: The interaction of HRG with FXIIa and polyP is predominantly mediated by the HRR domain. Like intact HRG, HRR downregulates the contact pathway and contributes to HRG-mediated down regulation of coagulation., (© 2021 International Society on Thrombosis and Haemostasis.)

Published

2022

18. Ablation of Plasma Prekallikrein Decreases Low-Density Lipoprotein Cholesterol by Stabilizing Low-Density Lipoprotein Receptor and Protects Against Atherosclerosis.

Author

Wang JK, Li Y, Zhao XL, Liu YB, Tan J, Xing YY, Adi D, Wang YT, Fu ZY, Ma YT, Liu SM, Liu Y, Wang Y, Shi XJ, Lu XY, Song BL, and Luo J

Subjects

Animals, Atherosclerosis genetics, Cholesterol, LDL genetics, Lysosomes genetics, Lysosomes metabolism, Mice, Mice, Knockout, Plaque, Atherosclerotic genetics, Prekallikrein metabolism, Proteolysis, Receptors, LDL genetics, Atherosclerosis metabolism, Atherosclerosis prevention & control, Cholesterol, LDL metabolism, Plaque, Atherosclerotic metabolism, Plaque, Atherosclerotic prevention & control, Prekallikrein deficiency, Receptors, LDL metabolism

Abstract

Background: High blood cholesterol accelerates the progression of atherosclerosis, which is an asymptomatic process lasting for decades. Rupture of atherosclerotic plaques induces thrombosis, which results in myocardial infarction or stroke. Lowering cholesterol levels is beneficial for preventing atherosclerotic cardiovascular disease., Methods: Low-density lipoprotein (LDL) receptor (LDLR) was used as bait to identify its binding proteins in the plasma, and the coagulation factor prekallikrein (PK; encoded by the KLKB1 gene) was revealed. The correlation between serum PK protein content and lipid levels in young Chinese Han people was then analyzed. To investigate the effects of PK ablation on LDLR and lipid levels in vivo, we genetically deleted Klkb1 in hamsters and heterozygous Ldlr knockout mice and knocked down Klkb1 using adeno-associated virus-mediated shRNA in rats. The additive effect of PK and proprotein convertase subtilisin/kexin 9 inhibition also was evaluated. In addition, we applied the anti-PK neutralizing antibody that blocked the PK and LDLR interaction in mice. Mice lacking both PK and apolipoprotein e ( Klkb1 -/- Apoe -/- ) were generated to assess the role of PK in atherosclerosis., Results: PK directly bound LDLR and induced its lysosomal degradation. The serum PK concentrations positively correlated with LDL cholesterol levels in 198 young Chinese Han adults. Genetic depletion of Klkb1 increased hepatic LDLR and decreased circulating cholesterol in multiple rodent models. Inhibition of proprotein convertase subtilisin/kexin 9 with evolocumab further decreased plasma LDL cholesterol levels in Klkb1 -deficient hamsters. The anti-PK neutralizing antibody could similarly lower plasma lipids through upregulating hepatic LDLR. Ablation of Klkb1 slowed the progression of atherosclerosis in mice on Apoe -deficient background., Conclusions: PK regulates circulating cholesterol levels through binding to LDLR and inducing its lysosomal degradation. Ablation of PK stabilizes LDLR, decreases LDL cholesterol, and prevents atherosclerotic plaque development. This study suggests that PK is a promising therapeutic target to treat atherosclerotic cardiovascular disease.

Published

2022

19. Skeletal muscle myosin promotes coagulation by binding factor XI via its A3 domain and enhancing thrombin-induced factor XI activation.

Author

Morla S, Deguchi H, Zilberman-Rudenko J, Gruber A, McCarty OJT, Srivastava P, Gailani D, and Griffin JH

Subjects

Antibodies, Monoclonal chemistry, Binding Sites, Prekallikrein chemistry, Prekallikrein metabolism, Protein Domains, Recombinant Fusion Proteins chemistry, Blood Coagulation, Factor XI chemistry, Factor XI genetics, Factor XI metabolism, Skeletal Muscle Myosins metabolism, Thrombin metabolism

Abstract

Skeletal muscle myosin (SkM) has been shown to possess procoagulant activity; however, the mechanisms of this coagulation-enhancing activity involving plasma coagulation pathways and factors are incompletely understood. Here, we discovered direct interactions between immobilized SkM and coagulation factor XI (FXI) using biolayer interferometry (K d  = 0.2 nM). In contrast, we show that prekallikrein, a FXI homolog, did not bind to SkM, reflecting the specificity of SkM for FXI binding. We also found that the anti-FXI monoclonal antibody, mAb 1A6, which recognizes the Apple (A) 3 domain of FXI, potently inhibited binding of FXI to immobilized SkM, implying that SkM binds FXI A3 domain. In addition, we show that SkM enhanced FXI activation by thrombin in a concentration-dependent manner. We further used recombinant FXI chimeric proteins in which each of the four A domains of the heavy chain (designated A1 through A4) was individually replaced with the corresponding A domain from prekallikrein to investigate SkM-mediated enhancement of thrombin-induced FXI activation. These results indicated that activation of two FXI chimeras with substitutions of either the A3 domains or A4 domains was not enhanced by SkM, whereas substitution of the A2 domain did not reduce the thrombin-induced activation compared with wildtype FXI. These data strongly suggest that functional interaction sites on FXI for SkM involve the A3 and A4 domains. Thus, this study is the first to reveal and support the novel intrinsic blood coagulation pathway concept that the procoagulant mechanisms of SkM include FXI binding and enhancement of FXI activation by thrombin., Competing Interests: Conflict of interest The authors declare that they have no conflicts of interest with the contents of this article., (Copyright © 2022 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2022

20. Effect of Anabolic-Androgenic Steroid Abuse on the Contact Activation System.

Author

Sidelmann JJ, Gram JB, Palarasah Y, Rasmussen JJ, and Kistorp C

Subjects

Adolescent, Adult, Biomarkers blood, Case-Control Studies, Complement C1 Inhibitor Protein metabolism, Cross-Sectional Studies, Factor XII metabolism, Female, Humans, Kallikreins blood, Kininogen, High-Molecular-Weight blood, Male, Middle Aged, Prekallikrein metabolism, Substance-Related Disorders complications, Substance-Related Disorders diagnosis, Young Adult, Androgens adverse effects, Blood Coagulation drug effects, Substance-Related Disorders blood, Testosterone Congeners adverse effects

Abstract

The effect of anabolic-androgenic steroid (AAS) abuse on the contact activation system (CAS) is not known in detail. We hypothesized that current AAS abuse reduces the kallikrein-generating capacity of CAS significantly and investigated the impact of AAS on the proteins and capacity of CAS in current and former AAS abusers and healthy age-matched controls. Men 18 to 50 years of age were included as current AAS abusers, former AAS abusers, or controls. Blood samples were collected after overnight fasting. Kallikrein generation (lag time, peak height, and endogenous kallikrein potential [EKP]), coagulation factor XII (FXII), prekallikrein, high-molecular-weight kininogen (HK), and Complement C1 esterase inhibitor (C1inh) were assessed. Groups were compared by analysis of variance or Kruskal-Wallis test and probabilities were corrected for multiple comparisons. Associations were evaluated by linear regression models. The EKP was significantly reduced in current ( n  = 37) AAS abusers (984 ± 328 nmol/L × min) compared with former ( n  = 33) abusers (1,543 ± 481 nmol/L × min) and controls ( n  = 30) (1,521 ± 339 nmol/L × min), p  < 0.001. Current abusers had higher levels of FXII and C1inh and lower levels of prekallikrein and HK than controls, p ≤ 0.025. Stepwise regression analysis showed that EKP was associated with C1inh and prekallikrein in current AAS abusers, R 2  = 0.70, p  < 0.001. We conclude that current AAS abuse reduces the kallikrein-generating capacity of CAS by increasing the concentration of C1inh and reducing the concentration of prekallikrein. These changes may contribute to the anti-inflammatory effect of testosterone., Competing Interests: None declared., (Thieme. All rights reserved.)

Published

2021

21. Analysis of cold activation of the contact system in hereditary angioedema with normal C1 inhibitor.

Author

Larrauri B, Hester CG, Jiang H, Miletic VD, Malbran A, Bork K, Kaplan A, and Frank M

Subjects

Adult, Bradykinin metabolism, Cold Temperature, Estrogens therapeutic use, Factor XII genetics, Female, Hereditary Angioedema Type III genetics, Humans, Kallikreins metabolism, Kininogens metabolism, Male, Middle Aged, Plasminogen genetics, Proteinase Inhibitory Proteins, Secretory metabolism, Young Adult, Blood Coagulation physiology, Complement C1 Inhibitor Protein metabolism, Factor XII metabolism, Hereditary Angioedema Type III immunology, Hereditary Angioedema Type III pathology, Prekallikrein metabolism

Abstract

Hereditary angioedema (HAE) attacks are caused by excessive activation of the contact system. Understanding how the contact system is activated in HAE, especially in patients with normal C1 inhibitor (HAEnCI), is essential to effectively treat this disease. Contact system activation involves the cleavage of several proteins including Factor XII (FXII), high molecular weight kininogen (HK), prekallikrein, sgp120 (ITIH4) and C1 inhibitor (C1-INH) before the subsequent generation of bradykinin that mediates HAE. In this study, we evaluated the fragmentation and enzymatic activity of contact system proteins in HAEnCI plasma samples before and after contact system activation induced by incubation in the cold. Our results show that in contrast to normal plasma, cold activation induced contact system activation in the majority of the HAEnCI patient samples we tested, in which each contact system protein exhibited fragmentation, FXII and kallikrein enzymatic activity increased, and C1-INH functional activity decreased. HAEnCI samples with low FXII concentrations or functional activity were not affected by cold activation. One HAEnCI sample with a plasminogen gene mutation activated the fibrinolytic system, as shown by an increase in concentration of plasma D dimers. Our results suggest that cold activation seems to be initiated by the cleavage of prekallikrein, and that it needs FXII in order to occur. Reported to be susceptible to excessive contact system activation after incubation in the cold, we further applied this system of study to the evaluation of plasma from women undergoing estrogen treatment. Similar to plasma from HAEnCI patients, excessive contact system activation was demonstrated., (Copyright © 2021. Published by Elsevier Ltd.)

Published

2021

22. Plasmin-mediated cleavage of high-molecular-weight kininogen contributes to acetaminophen-induced acute liver failure.

Author

Henderson MW, Sparkenbaugh EM, Wang S, Ilich A, Noubouossie DF, Mailer R, Renné T, Flick MJ, Luyendyk JP, Chen ZL, Strickland S, Stravitz RT, McCrae KR, Key NS, and Pawlinski R

Subjects

Acetaminophen pharmacology, Animals, Chemical and Drug Induced Liver Injury genetics, Chemical and Drug Induced Liver Injury pathology, Factor XII genetics, Factor XII metabolism, Female, Fibrinolysin genetics, Humans, Kininogens genetics, Male, Mice, Mice, Knockout, Prekallikrein genetics, Prekallikrein metabolism, Acetaminophen adverse effects, Chemical and Drug Induced Liver Injury metabolism, Fibrinolysin metabolism, Fibrinolysis drug effects, Kininogens metabolism, Proteolysis drug effects

Abstract

Acetaminophen (APAP)-induced liver injury is associated with activation of coagulation and fibrinolysis. In mice, both tissue factor-dependent thrombin generation and plasmin activity have been shown to promote liver injury after APAP overdose. However, the contribution of the contact and intrinsic coagulation pathways has not been investigated in this model. Mice deficient in individual factors of the contact (factor XII [FXII] and prekallikrein) or intrinsic coagulation (FXI) pathway were administered a hepatotoxic dose of 400 mg/kg of APAP. Neither FXII, FXI, nor prekallikrein deficiency mitigated coagulation activation or hepatocellular injury. Interestingly, despite the lack of significant changes to APAP-induced coagulation activation, markers of liver injury and inflammation were significantly reduced in APAP-challenged high-molecular-weight kininogen-deficient (HK-/-) mice. Protective effects of HK deficiency were not reproduced by inhibition of bradykinin-mediated signaling, whereas reconstitution of circulating levels of HK in HK-/- mice restored hepatotoxicity. Fibrinolysis activation was observed in mice after APAP administration. Western blotting, enzyme-linked immunosorbent assay, and mass spectrometry analysis showed that plasmin efficiently cleaves HK into multiple fragments in buffer or plasma. Importantly, plasminogen deficiency attenuated APAP-induced liver injury and prevented HK cleavage in the injured liver. Finally, enhanced plasmin generation and HK cleavage, in the absence of contact pathway activation, were observed in plasma of patients with acute liver failure due to APAP overdose. In summary, extrinsic but not intrinsic pathway activation drives the thromboinflammatory pathology associated with APAP-induced liver injury in mice. Furthermore, plasmin-mediated cleavage of HK contributes to hepatotoxicity in APAP-challenged mice independently of thrombin generation or bradykinin signaling., (© 2021 by The American Society of Hematology.)

Published

2021

23. Proteolytic activity of contact factor zymogens.

Author

Shamanaev A, Emsley J, and Gailani D

Subjects

Factor XI metabolism, Humans, Prekallikrein metabolism, Proteolysis, Enzyme Precursors, Factor XII metabolism

Abstract

Contact activation is triggered when blood is exposed to compounds or "surfaces" that promote conversion of the plasma zymogens factor XII (FXII) and prekallikrein to the active proteases FXIIa and kallikrein. FXIIa promotes blood coagulation by converting zymogen factor XI (FXI) to the protease FXIa. Contact activation appears to represent an enhancement of the propensity for FXII and prekallikrein to reciprocally activate each other by surface-independent limited proteolysis. The nature of the activities that perpetuate this process, and that trigger contact activation, are debated. FXII and prekallikrein, like most members of the chymotrypsin/trypsin protease family, are synthesized as single polypeptides that are presumed to be in an inactive state. Internal cleavage leads to conformational changes in the protease domain that convert the enzyme active site from a closed conformation to an open conformation accessible to substrates. We observed that FXII expresses a low level of activity as a single-chain zymogen that catalyzes prekallikrein activation in solution, as well as surface-dependent activation of prekallikrein, FXI, and FXII (autoactivation). Prekallikrein also expresses activity that promotes cleavage of kininogen to release bradykinin, and surface-dependent FXII activation. Modeling suggests that a glutamine residue at position 156 in the FXII and prekallikrein protease domains stabilizes an open active site conformation by forming hydrogen bonds with Asp194. The activity inherent in FXII and prekallikrein suggests a mechanism for sustaining reciprocal activation of the proteins and for initiating contact activation, and supports the premise that zymogens of some trypsin-like enzymes are active proteases., (© 2020 International Society on Thrombosis and Haemostasis.)

Published

2021

24. Development of an updated assay for prekallikrein activator in albumin and immunoglobulin therapeutics.

Author

Roberts G, Fox B, and Longstaff C

Subjects

Factor XIIa metabolism, Humans, Prekallikrein metabolism, Reproducibility of Results, Albumins, Factor XIIa analysis, Immunoglobulins

Abstract

Background: Prekallikrein activator (PKA) is a contaminating enzyme found in therapeutic albumin and immunoglobulin products. The level is commonly measured using methods such as that defined by the European Pharmacopoeia (Ph Eur) with traceability to the WHO International Standard for PKA. This method generally works well, but problems are sometimes observed., Materials and Methods: A simplified one-step method has been developed to replace the existing Ph Eur two-step method which consists of kallikrein generation followed by kallikrein measurement using a chromogenic substrate. Analysis of data from the one-stage method is simplified by the use of a dedicated online app., Results: The one-stage method was validated against the current Ph Eur method using batches of albumin and immunoglobulins. Problem batches of immunoglobulins were investigated using the one-stage method. Improved methodology using true initial rate determinations and use of acid-treated prekallikrein substrate (PKS) helped understand and reduce artefactual results., Conclusions: The one-stage method and associated app streamline real-time determination of PKA and promote good principles of enzyme assays to limit substrate depletion, while also conserving expensive PKS. Blanking steps and reproducibility are simplified., (© 2020 Crown copyright. Vox Sanguinis published by John Wiley & Sons Ltd on behalf of International Society of Blood Transfusion. This article is published with the permission of the controller of HMSO and the Queen’s Printer for Scotland.)

Published

2021

25. The evolution of factor XI and the kallikrein-kinin system.

Author

Ponczek MB, Shamanaev A, LaPlace A, Dickeson SK, Srivastava P, Sun MF, Gruber A, Kastrup C, Emsley J, and Gailani D

Subjects

Animals, Factor XIIa metabolism, Female, Humans, Kallikrein-Kinin System, Pregnancy, Prekallikrein genetics, Prekallikrein metabolism, Factor XI genetics, Factor XI metabolism, Factor XI Deficiency genetics

Abstract

Factor XI (FXI) is the zymogen of a plasma protease (FXIa) that contributes to hemostasis by activating factor IX (FIX). In the original cascade model of coagulation, FXI is converted to FXIa by factor XIIa (FXIIa), a component, along with prekallikrein and high-molecular-weight kininogen (HK), of the plasma kallikrein-kinin system (KKS). More recent coagulation models emphasize thrombin as a FXI activator, bypassing the need for FXIIa and the KKS. We took an evolutionary approach to better understand the relationship of FXI to the KKS and thrombin generation. BLAST searches were conducted for FXI, FXII, prekallikrein, and HK using genomes for multiple vertebrate species. The analysis shows the KKS appeared in lobe-finned fish, the ancestors of all land vertebrates. FXI arose later from a duplication of the prekallikrein gene early in mammalian evolution. Features of FXI that facilitate efficient FIX activation are present in all living mammals, including primitive egg-laying monotremes, and may represent enhancement of FIX-activating activity inherent in prekallikrein. FXI activation by thrombin is a more recent acquisition, appearing in placental mammals. These findings suggest FXI activation by FXIIa may be more important to hemostasis in primitive mammals than in placental mammals. FXI activation by thrombin places FXI partially under control of the vitamin K-dependent coagulation mechanism, reducing the importance of the KKS in blood coagulation. This would explain why humans with FXI deficiency have a bleeding abnormality, whereas those lacking components of the KKS do not., (© 2020 by The American Society of Hematology.)

Published

2020

26. Severe high-molecular-weight kininogen deficiency due to a homozygous c.1456C > T nonsense variant in a large Chinese family.

Author

Yang J, Fan L, Qiao Y, Zhao Y, and Zhu T

Subjects

Aged, Asian People, Asymptomatic Diseases, Blood Coagulation Tests methods, Codon, Nonsense, Family, Female, Homozygote, Humans, Kininogen, High-Molecular-Weight blood, Kininogen, High-Molecular-Weight genetics, Male, Medical History Taking, Middle Aged, Partial Thromboplastin Time methods, Pedigree, Prekallikrein metabolism, Blood Coagulation Disorders blood, Blood Coagulation Disorders diagnosis, Blood Coagulation Disorders genetics, Kininogen, High-Molecular-Weight deficiency

Abstract

High-molecular-weight kininogen (HMWK) deficiency is a very rare hereditary disorder caused by a defect of Kininogen-1 gene (KGN1). A 67-year-old asymptomatic male with an isolated prolonged activated partial thromboplastin time (aPTT) was recognized to have HMWK deficiency. The propositus had less than 1% HMWK procoagulant activity. The plasma HMWK procoagulant activities of his 2 younger sisters were 1.1% and less than 1%, respectively. Prekallikrein (PK) activity was also reduced in the propositus and two of his younger sisters with severe HMWK deficiency. Genetic testing to identify the KGN1 mutation provides a precise diagnosis for the patient and other family members. This Chinese family has a novel KGN1 nonsense variant, C to T, at nucleotide position 1456 leading to a stop codon in position 486 (p. Gln486*).

Published

2020

27. Novel anti-thrombotic mechanisms mediated by Mas receptor as result of balanced activities between the kallikrein/kinin and the renin-angiotensin systems.

Author

Fang C and Schmaier AH

Subjects

Animals, Epoprostenol metabolism, Humans, Prekallikrein metabolism, Proto-Oncogene Mas, Receptor, Bradykinin B2 metabolism, Signal Transduction, Sirtuin 1 metabolism, Blood Coagulation, Kallikrein-Kinin System drug effects, Proto-Oncogene Proteins metabolism, Receptors, G-Protein-Coupled metabolism, Renin-Angiotensin System, Thrombosis blood

Abstract

The risk of thrombosis, a globally growing challenge and a major cause of death, is influenced by various factors in the intravascular coagulation, vessel wall, and cellular systems. Among the contributors to thrombosis, the contact activation system and the kallikrein/kinin system, two overlapping plasma proteolytic systems that are often considered as synonymous, regulate thrombosis from different aspects. On one hand, components of the contact activation system such as factor XII initiates activation of the coagulation proteins promoting thrombus formation on artificial surfaces through factor XI- and possibly prekallikrein-mediated intrinsic coagulation. On the other hand, physiological activation of plasma prekallikrein in the kallikrein/kinin system on endothelial cells liberates bradykinin from associated high-molecular-weight kininogen to stimulate the constitutive bradykinin B2 receptor to generate nitric oxide and prostacyclin to induce vasodilation and counterbalance angiotensin II signaling from the renin-angiotensin system which stimulates vasoconstriction. In addition to vascular tone regulation, this interaction between the kallikrein/kinin and renin-angiotensin systems has a thrombo-regulatory role independent of the contact pathway. At the level of the G-protein coupled receptors of these systems, defective bradykinin signaling due to attenuated bradykinin formation and/or decreased B2 receptor expression, as seen in murine prekallikrein and B2 receptor null mice, respectively, leads to compensatory overexpressed Mas, the receptor for angiotensin-(1-7) of the renin-angiotensin system. Mas stimulation and/or its increased expression contributes to maintaining a healthy vascular homeostasis by generating graded elevation of plasma prostacyclin which reduces thrombosis through two independent pathways: (1) increasing the vasoprotective transcription factor Sirtuin 1 to suppress tissue factor expression, and (2) inhibiting platelet activation. This review will summarize the recent advances in this field that support these understandings. Appreciating these subtle mechanisms help to develop novel anti-thrombotic strategies by targeting the vascular receptors in the renin-angiotensin and the kallikrein/kinin systems to maintain healthy vascular homeostasis., (Copyright © 2020 Elsevier Ltd. All rights reserved.)

Published

2020

28. Antisense Inhibition of Prekallikrein to Control Hereditary Angioedema.

Author

Cohn DM, Viney NJ, Fijen LM, Schneider E, Alexander VJ, Xia S, Kaeser GE, Nanavati C, Baker BF, Geary RS, Levi M, Meijers JCM, and Stroes ESG

Subjects

Adult, Angioedemas, Hereditary metabolism, Bradykinin metabolism, Compassionate Use Trials, Female, Humans, Injections, Subcutaneous, Oligonucleotides, Antisense administration & dosage, Pilot Projects, Prekallikrein metabolism, Angioedemas, Hereditary drug therapy, Oligonucleotides, Antisense therapeutic use, Prekallikrein antagonists & inhibitors

Abstract

Hereditary angioedema is characterized by recurrent and unpredictable episodes of subcutaneous and mucosal swelling that can be life threatening. IONIS-PKK-L Rx is a ligand-conjugated antisense oligonucleotide designed for receptor-mediated delivery to hepatocytes. In a compassionate-use pilot study, two patients with severe bradykinin-mediated angioedema were initially administered weekly subcutaneous injections of the unconjugated parent drug, IONIS-PKK Rx , for 12 to 16 weeks, after which they received IONIS-PKK-L Rx at a dose of 80 mg every 3 to 4 weeks for 7 to 8 months. Treatment was accompanied by a reduction in the angioedema attack rate. (Funded by Amsterdam UMC.)., (Copyright © 2020 Massachusetts Medical Society.)

Published

2020

29. Understanding the Pathophysiology of COVID-19: Could the Contact System Be the Key?

Author

Meini S, Zanichelli A, Sbrojavacca R, Iuri F, Roberts AT, Suffritti C, and Tascini C

Subjects

Angiotensin-Converting Enzyme 2, Bradykinin metabolism, COVID-19, Capillary Permeability, Complement C1 Inhibitor Protein, Coronavirus Infections virology, Factor XIIa metabolism, Host-Pathogen Interactions immunology, Humans, Kininogen, High-Molecular-Weight metabolism, Pandemics, Peptidyl-Dipeptidase A metabolism, Plasma Kallikrein metabolism, Pneumonia, Viral virology, Prekallikrein metabolism, Receptor, Bradykinin B1 metabolism, Receptor, Bradykinin B2 metabolism, SARS-CoV-2, Vasodilation, Betacoronavirus metabolism, Coronavirus Infections immunology, Coronavirus Infections physiopathology, Fibrinolysis immunology, Kallikrein-Kinin System immunology, Pneumonia, Viral immunology, Pneumonia, Viral physiopathology, Renin-Angiotensin System immunology

Abstract

To date the pathophysiology of COVID-19 remains unclear: this represents a factor determining the current lack of effective treatments. In this paper, we hypothesized a complex host response to SARS-CoV-2, with the Contact System (CS) playing a pivotal role in innate immune response. CS is linked with different proteolytic defense systems operating in human vasculature: the Kallikrein-Kinin (KKS), the Coagulation/Fibrinolysis and the Renin-Angiotensin (RAS) Systems. We investigated the role of the mediators involved. CS consists of Factor XII (FXII) and plasma prekallikrein (complexed to high-molecular-weight kininogen-HK). Autoactivation of FXII by contact with SARS-CoV-2 could lead to activation of intrinsic coagulation, with fibrin formation (microthrombosis), and fibrinolysis, resulting in increased D-dimer levels. Activation of kallikrein by activated FXII leads to production of bradykinin (BK) from HK. BK binds to B2-receptors, mediating vascular permeability, vasodilation and edema. B1-receptors, binding the metabolite [des-Arg 9 ]-BK (DABK), are up-regulated during infections and mediate lung inflammatory responses. BK could play a relevant role in COVID-19 as already described for other viral models. Angiotensin-Converting-Enzyme (ACE) 2 displays lung protective effects: it inactivates DABK and converts Angiotensin II (Ang II) into Angiotensin-(1-7) and Angiotensin I into Angiotensin-(1-9). SARS-CoV-2 binds to ACE2 for cell entry, downregulating it: an impaired DABK inactivation could lead to an enhanced activity of B1-receptors, and the accumulation of Ang II, through a negative feedback loop, may result in decreased ACE activity, with consequent increase of BK. Therapies targeting the CS, the KKS and action of BK could be effective for the treatment of COVID-19., (Copyright © 2020 Meini, Zanichelli, Sbrojavacca, Iuri, Roberts, Suffritti and Tascini.)

Published

2020

30. Role of Factor XIa and Plasma Kallikrein in Arterial and Venous Thrombosis.

Author

Visser M, Heitmeier S, Ten Cate H, and Spronk HMH

Subjects

Animals, Blood Coagulation physiology, Blood Coagulation Disorders blood, Blood Coagulation Factors physiology, Disease Models, Animal, Enzyme Activation, Factor XI Deficiency blood, Factor XIa chemistry, Factor XIa immunology, Factor Xa Inhibitors therapeutic use, Humans, Mice, Mice, Knockout, Prekallikrein deficiency, Prekallikrein metabolism, Protein Processing, Post-Translational, Species Specificity, Thrombophilia drug therapy, Venous Thrombosis blood, Arterial Occlusive Diseases blood, Factor XIa physiology, Plasma Kallikrein physiology, Thrombosis blood

Abstract

Cardiovascular disease, including stroke, myocardial infarction, and venous thromboembolism, is one of the leading causes of morbidity and mortality worldwide. Excessive coagulation may cause vascular occlusion in arteries and veins eventually leading to thrombotic diseases. Studies in recent years suggest that coagulation factors are involved in these pathological mechanisms. Factors XIa (FXIa), XIIa (FXIIa), and plasma kallikrein (PKa) of the contact system of coagulation appear to contribute to thrombosis while playing a limited role in hemostasis. Contact activation is initiated upon autoactivation of FXII on negatively charged surfaces. FXIIa activates plasma prekallikrein (PK) to PKa, which in turn activates FXII and initiates the kallikrein-kinin pathway. FXI is also activated by FXIIa, leading to activation of FIX and finally to thrombin formation, which in turn activates FXI in an amplification loop. Animal studies have shown that arterial and venous thrombosis can be reduced by the inhibition of FXI(a) or PKa. Furthermore, data from human studies suggest that these enzymes may be valuable targets to reduce thrombosis risk. In this review, we discuss the structure and function of FXI(a) and PK(a), their involvement in the development of venous and arterial thrombosis in animal models and human studies, and current therapeutic strategies., Competing Interests: S.H. is an employee of Bayer AG, Germany. M.V., H.T.C. and H.M.H.S. have nothing to disclose. H.T.C. was a fellow of the Gutenberg Research Foundation and is adjunct professor at the Center for Thrombosis and Hemostasis, Gutenberg University, Mainz, Germany. H.M.H.S. and H.T.C. receive support from the Netherlands Heart Foundation: CVON2014-09, reappraisal of atrial fibrillation: interaction between hypercoagulability, electrical remodeling, and vascular destabilization in the progression of atrial fibrillation (RACE V)., (Georg Thieme Verlag KG Stuttgart · New York.)

Published

2020

31. Protease activity in single-chain prekallikrein.

Author

Ivanov I, Verhamme IM, Sun MF, Mohammed B, Cheng Q, Matafonov A, Dickeson SK, Joseph K, Kaplan AP, and Gailani D

Subjects

Amino Acid Substitution, Animals, Factor XII metabolism, HEK293 Cells, Humans, Kininogen, High-Molecular-Weight metabolism, Mice, Inbred C57BL, Prekallikrein chemistry, Prekallikrein genetics, Proteolysis, Recombinant Proteins chemistry, Recombinant Proteins genetics, Recombinant Proteins metabolism, Blood Coagulation, Bradykinin metabolism, Prekallikrein metabolism

Abstract

Prekallikrein (PK) is the precursor of the trypsin-like plasma protease kallikrein (PKa), which cleaves kininogens to release bradykinin and converts the protease precursor factor XII (FXII) to the enzyme FXIIa. PK and FXII undergo reciprocal conversion to their active forms (PKa and FXIIa) by a process that is accelerated by a variety of biological and artificial surfaces. The surface-mediated process is referred to as contact activation. Previously, we showed that FXII expresses a low level of proteolytic activity (independently of FXIIa) that may initiate reciprocal activation with PK. The current study was undertaken to determine whether PK expresses similar activity. Recombinant PK that cannot be converted to PKa was prepared by replacing Arg371 with alanine at the activation cleavage site (PK-R371A, or single-chain PK). Despite being constrained to the single-chain precursor form, PK-R371A cleaves high-molecular-weight kininogen (HK) to release bradykinin with a catalytic efficiency ∼1500-fold lower than that of kallikrein cleavage of HK. In the presence of a surface, PK-R371A converts FXII to FXIIa with a specific activity ∼4 orders of magnitude lower than for PKa cleavage of FXII. These results support the notion that activity intrinsic to PK and FXII can initiate reciprocal activation of FXII and PK in solution or on a surface. The findings are consistent with the hypothesis that the putative zymogens of many trypsin-like proteases are actually active proteases, explaining their capacity to undergo processes such as autoactivation and to initiate enzyme cascades., (© 2020 by The American Society of Hematology.)

Published

2020

32. Prekallikrein inhibits innate immune signaling in the lung and impairs host defense during pneumosepsis in mice.

Author

Ding C, Scicluna BP, Stroo I, Yang J, Roelofs JJ, de Boer OJ, de Vos AF, Nürnberg P, Revenko AS, Crosby J, Van't Veer C, and van der Poll T

Subjects

Animals, Disease Models, Animal, Klebsiella Infections immunology, Klebsiella Infections microbiology, Klebsiella Infections prevention & control, Klebsiella pneumoniae immunology, Lung immunology, Lung microbiology, Male, Mice, Inbred C57BL, Oligonucleotides, Antisense administration & dosage, Pneumonia, Bacterial immunology, Pneumonia, Bacterial microbiology, Pneumonia, Bacterial prevention & control, Prekallikrein genetics, Sepsis immunology, Sepsis microbiology, Sepsis prevention & control, Signal Transduction, Immunity, Innate, Klebsiella Infections enzymology, Klebsiella pneumoniae pathogenicity, Lung enzymology, Pneumonia, Bacterial enzymology, Prekallikrein metabolism, Sepsis enzymology

Abstract

Prekallikrein (PKK, also known as Fletcher factor and encoded by the gene KLKB1 in humans) is a component of the contact system. Activation of the contact system has been implicated in lethality in fulminant sepsis models. Pneumonia is the most frequent cause of sepsis. We sought to determine the role of PKK in host defense during pneumosepsis. To this end, mice were infected with the common human pathogen Klebsiella pneumoniae via the airways, causing an initially localized infection of the lungs with subsequent bacterial dissemination and sepsis. Mice were treated with a selective PKK-directed antisense oligonucleotide (ASO) or a scrambled control ASO for 3 weeks prior to infection. Host response readouts were determined at 12 or 36 h post-infection, including genome-wide messenger RNA profiling of lungs, or mice were followed for survival. PKK ASO treatment inhibited constitutive hepatic Klkb1 mRNA expression by >80% and almost completely abolished plasma PKK activity. Klkb1 mRNA could not be detected in lungs. Pneumonia was associated with a progressive decline in PKK expression in mice treated with control ASO. PKK ASO administration was associated with a delayed mortality, reduced bacterial burdens, and diminished distant organ injury. While PKK depletion did not influence lung pathology or neutrophil recruitment, it was associated with an upregulation of multiple innate immune signaling pathways in the lungs already prior to infection. Activation of the contact system could not be detected, either during infection in vivo or at the surface of Klebsiella in vitro. These data suggest that circulating PKK confines pro-inflammatory signaling in the lung by a mechanism that does not involve contact system activation, which in the case of respiratory tract infection may impede early protective innate immunity. © 2019 Authors. Journal of Pathology published by John Wiley & Sons Ltd on behalf of Pathological Society of Great Britain and Ireland., (© 2019 Authors. Journal of Pathology published by John Wiley & Sons Ltd on behalf of Pathological Society of Great Britain and Ireland.)

Published

2020

33. Nomenclature of factor XI and the contact system.

Author

Schmaier AH, Emsley J, Feener EP, Gailani D, Govers-Riemslag JWP, Kaplan AP, Maas C, Morrissey JH, Renné T, Sidelmann JJ, and Meijers JCM

Subjects

Consensus, Factor XI chemistry, Factor XII chemistry, Factor XII classification, Factor XII metabolism, Humans, Kininogen, High-Molecular-Weight chemistry, Kininogen, High-Molecular-Weight classification, Kininogen, High-Molecular-Weight metabolism, Molecular Structure, Prekallikrein chemistry, Prekallikrein classification, Prekallikrein metabolism, Structure-Activity Relationship, Blood Coagulation, Factor XI classification, Factor XI metabolism, Terminology as Topic

Published

2019

34. A non-circulating pool of factor XI associated with glycosaminoglycans in mice.

Author

Mohammed BM, Cheng Q, Matafonov A, Verhamme IM, Emsley J, McCrae KR, McCarty OJT, Gruber A, and Gailani D

Subjects

Animals, Binding Sites, Carotid Artery Thrombosis blood, Carotid Artery Thrombosis chemically induced, Chlorides toxicity, Factor XI chemistry, Factor XI Deficiency blood, Ferric Compounds toxicity, Heparin pharmacology, Humans, Kininogens blood, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Models, Molecular, Papio, Prekallikrein metabolism, Protein Binding, Protein Conformation, Rats, Rats, Sprague-Dawley, Recombinant Proteins metabolism, Sequence Alignment, Species Specificity, Static Electricity, Endothelium, Vascular metabolism, Factor XI metabolism, Glycosaminoglycans blood

Abstract

Background: The homologous plasma proteins prekallikrein and factor XI (FXI) circulate as complexes with high molecular weight kininogen. Although evidence supports an interaction between the prekallikrein-kininogen complexes and vascular endothelium, there is conflicting information regarding FXI binding to endothelium., Objective: To study the interaction between FXI and blood vessels in mice., Methods: C57Bl/6 wild-type or F11-/- mice in which variants of FXI were expressed by hydrodynamic tail vein injection, received intravenous infusions of saline, heparin, polyphosphates, protamine, or enzymes that digest glycosaminoglycans (GAGs). Blood was collected after infusion and plasma was analyzed by western blot for FXI., Results and Conclusions: Plasma FXI increased 5- to 10-fold in wild-type mice after infusion of heparin, polyphosphates, protamine, or GAG-digesting enzymes, but not saline. Similar treatments resulted in a much smaller change in plasma FXI levels in rats, and infusions of large boluses of heparin did not change FXI levels appreciably in baboons or humans. The releasable FXI fraction was reconstituted in F11-/- mice by expressing murine FXI, but not human FXI. We identified a cluster of basic residues on the apple 4 domain of mouse FXI that is not present in other species. Replacing the basic residues with alanine prevented the interaction of mouse FXI with blood vessels, whereas introducing the basic residues into human FXI allowed it to bind to blood vessels. Most FXI in mice is noncovalently associated with GAGs on blood vessel endothelium and does not circulate in plasma., (© 2019 International Society on Thrombosis and Haemostasis.)

Published

2019

35. Plasma kallikrein structure reveals apple domain disc rotated conformation compared to factor XI.

Author

Li C, Voos KM, Pathak M, Hall G, McCrae KR, Dreveny I, Li R, and Emsley J

Subjects

Binding Sites, Bradykinin chemistry, Humans, Inflammation, Kininogens chemistry, Mutation, Prekallikrein metabolism, Protein Binding, Protein Domains, Protein Multimerization, Recombinant Proteins chemistry, Thrombosis, Factor XI chemistry, Plasma Kallikrein chemistry

Abstract

Essentials Zymogen PK is activated to PKa and cleaves substrates kininogen and FXII contributing to bradykinin generation. Monomeric PKa and dimeric homologue FXI utilize the N-terminal apple domains to recruit substrates. A high-resolution 1.3 Å structure of full-length PKa reveals an active conformation of the protease and apple domains. The PKa protease and four-apple domain disc organization is 180° rotated compared to FXI. SUMMARY: Background Plasma prekallikrein (PK) and factor XI (FXI) are apple domain-containing serine proteases that when activated to PKa and FXIa cleave substrates kininogen, factor XII, and factor IX, respectively, directing plasma coagulation, bradykinin release, inflammation, and thrombosis pathways. Objective To investigate the three-dimensional structure of full-length PKa and perform a comparison with FXI. Methods A series of recombinant full-length PKa and FXI constructs and variants were developed and the crystal structures determined. Results and conclusions A 1.3 Å structure of full-length PKa reveals the protease domain positioned above a disc-shaped assemblage of four apple domains in an active conformation. A comparison with the homologous FXI structure reveals the intramolecular disulfide and structural differences in the apple 4 domain that prevents dimer formation in PK as opposed to FXI. Two latchlike loops (LL1 and LL2) extend from the PKa protease domain to form interactions with the apple 1 and apple 3 domains, respectively. A major unexpected difference in the PKa structure compared to FXI is the 180° disc rotation of the apple domains relative to the protease domain. This results in a switched configuration of the latch loops such that LL2 interacts and buries portions of the apple 3 domain in the FXI zymogen whereas in PKa LL2 interacts with the apple 1 domain. Hydrogen-deuterium exchange mass spectrometry on plasma purified human PK and PKa determined that regions of the apple 3 domain have increased surface exposure in PKa compared to the zymogen PK, suggesting conformational change upon activation., (© 2019 The Authors. Journal of Thrombosis and Haemostasis published by Wiley Periodicals, Inc. on behalf of International Society on Thrombosis and Haemostasis.)

Published

2019

36. Plasma Concentrations of High Molecular Weight Kininogen and Prekallikrein and Venous Thromboembolism Incidence in the General Population.

Author

Folsom AR, Tang W, Basu S, Misialek JR, Couper D, Heckbert SR, and Cushman M

Subjects

Blood Coagulation, Case-Control Studies, Cohort Studies, Female, Follow-Up Studies, Humans, Incidence, Kallikrein-Kinin System, Male, Middle Aged, Prospective Studies, Risk, United States epidemiology, Venous Thromboembolism epidemiology, Kininogen, High-Molecular-Weight blood, Plasma metabolism, Population Groups, Prekallikrein metabolism, Venous Thromboembolism metabolism

Abstract

The kallikrein/kinin system, an intravascular biochemical pathway that includes several proteins involved in the contact activation system of coagulation, renin-angiotensin activation and inflammation, may or may not play a role in venous thromboembolism (VTE) occurrence. Within a large prospective population-based study in the United States, we conducted a nested case-cohort study to test the hypothesis that higher plasma levels of high molecular weight kininogen (HK) or prekallikrein are associated with greater VTE incidence. We related baseline enzyme-linked immunosorbent assay measures of HK and prekallikrein in 1993 to 1995 to incidence VTE of the lower extremity ( n  = 612) through 2015 (mean follow-up = 18 years). We found no evidence that plasma HK or prekallikrein was associated positively with incident VTE. HK, in fact, was associated inversely and significantly with VTE in most proportional hazards regression models. For example, the hazard ratio of VTE per standard deviation higher HK concentration was 0.88 (95% confidence interval = 0.81, 0.97), after adjustment for several VTE risk factors. Our findings suggest that plasma levels of these factors do not determine the risk of VTE in the general population., Competing Interests: None declared., (Georg Thieme Verlag KG Stuttgart · New York.)

Published

2019

37. Genetic determinants of activity and antigen levels of contact system factors.

Author

Rohmann JL, de Haan HG, Algra A, Vossen CY, Rosendaal FR, and Siegerink B

Subjects

Adolescent, Adult, Blood Coagulation Factors metabolism, Brain Ischemia blood, Brain Ischemia epidemiology, Brain Ischemia genetics, Case-Control Studies, Female, Genetic Predisposition to Disease, Humans, Kallikreins metabolism, Kininogen, High-Molecular-Weight blood, Kininogens blood, Middle Aged, Myocardial Infarction blood, Myocardial Infarction epidemiology, Myocardial Infarction genetics, Netherlands epidemiology, Phenotype, Prekallikrein genetics, Prekallikrein metabolism, Risk Factors, Stroke blood, Stroke epidemiology, Stroke genetics, Thrombosis blood, Thrombosis epidemiology, Young Adult, Blood Coagulation genetics, Blood Coagulation Factors genetics, Kallikreins genetics, Kininogen, High-Molecular-Weight genetics, Kininogens genetics, Polymorphism, Single Nucleotide, Thrombosis genetics

Abstract

Essentials Genetic variation may provide valuable insight into the role of the contact system in thrombosis. Explored associations of genetic variants with activity, antigen, and disease in RATIO study. Two novel loci were identified: KLKB1 rs4253243 for prekallikrein; KNG1 rs5029980 for HMWK levels. Contact system variants and haplotypes were not associated with myocardial infarction or stroke. SUMMARY: Background The complex, interdependent contact activation system has been implicated in thrombotic disease, although few genetic determinants of levels of proteins from this system are known. Objectives Our primary aim was to study the influence of common F11, F12, KLKB1, and KNG1 variants on factor (F) XI activity and FXI, FXII, prekallikrein (PK) and high-molecular-weight kininogen (HMWK) antigen levels, as well as the risk of myocardial infarction and ischemic stroke. Patients/methods We analyzed samples from all 630 healthy participants, 182 ischemic stroke patients and 216 myocardial infarction patients in the RATIO case-control study of women aged < 50 years. Forty-three tagging single nucleotide variants (SNVs) were genotyped to represent common genetic variation in the contact system genes. Antigen and activity levels were measured with sandwich-ELISA-based and one-stage clotting assays. We performed single variant, age-adjusted, linear regression analyses per trait and disease phenotype, assuming additive inheritance and determined conditionally independent associations. Haplotypes based on the lead SNV and all conditionally independent SNVs were tested for association with traits and disease. Results We identified two novel associations of KLKB1 SNV rs4253243 with PK antigen (β conditional = -12.38; 95% CI, -20.07 to -4.69) and KNG1 SNV rs5029980 with HMWK antigen (β conditional = 5.86; 95% CI, 2.40-9.32) and replicated previously reported associations in a single study. Further analyses probed whether the observed associations were indicative of linkage, pleiotropic effects or mediation. No individual SNVs or haplotypes were associated with the disease outcomes. Conclusion This study adds to current knowledge of how genetic variation influences contact system protein levels and clarifies interdependencies., (© 2018 International Society on Thrombosis and Haemostasis.)

Published

2019

38. Factor XII in coagulation, inflammation and beyond.

Author

Didiasova M, Wujak L, Schaefer L, and Wygrecka M

Subjects

Animals, Atherosclerosis immunology, Bradykinin metabolism, Cell Movement, Cell Proliferation, Complement Pathway, Classical immunology, Factor XI metabolism, Fibrinolysis immunology, Fibroblasts immunology, Humans, Kininogen, High-Molecular-Weight metabolism, Mice, Neutrophils immunology, Plasma Kallikrein metabolism, Prekallikrein metabolism, Wound Healing immunology, Blood Coagulation immunology, Factor XII chemistry, Factor XII physiology, Inflammation immunology, Inflammation metabolism

Abstract

Factor XII (FXII) is a protease that is mainly produced in the liver and circulates in plasma as a single chain zymogen. Following contact with negatively charged surfaces, FXII is converted into the two-chain active form, FXIIa. FXIIa initiates the intrinsic blood coagulation pathway via activation of factor XI. Furthermore, it converts plasma prekallikrein to kallikrein (PK), which reciprocally activates FXII and liberates bradykinin from high molecular weight kininogen. In addition, FXIIa initiates fibrinolysis via PK-mediated urokinase activation and activates the classical complement pathway. Even though the main function of FXII seems to relate to the activation of the intrinsic coagulation pathway and the kallikrein-kinin system, a growing body of evidence suggests that FXII may also directly regulate cellular responses. In this regard, it has been found that FXII/FXIIa induces the expression of inflammatory mediators, promotes cell proliferation, and enhances the migration of neutrophils and lung fibroblasts. In addition, it has been reported that genetic ablation of FXII protects against neuroinflammation, reduces the formation of atherosclerotic lesions in Apoe -/- mice, improves wound healing, and inhibits postnatal angiogenesis. Although the aforementioned effects can be partially explained by the downstream products of FXII activation, the ability of FXII/FXIIa to directly regulate cellular responses has recently emerged as an alternative hypothesis. These direct cellular reactions to FXII/FXIIa will be discussed in the review., (Copyright © 2018 Elsevier Inc. All rights reserved.)

Published

2018

39. Plasma contact activation by a fucosylated chondroitin sulfate and its structure-activity relationship study.

Author

Lin L, Xu L, Xiao C, Zhou L, Gao N, Wu M, and Zhao J

Subjects

Chondroitin Sulfates chemistry, Factor XIIa chemistry, Humans, Kininogens chemistry, Prekallikrein chemistry, Structure-Activity Relationship, Chondroitin Sulfates blood, Chondroitin Sulfates metabolism, Factor XIIa metabolism, Kininogens metabolism, Prekallikrein metabolism

Abstract

Plasma contact system is the initial part of both the intrinsic coagulation pathway and kallikrein-kinin pathway, which mainly involves three proteins: coagulation factor XII (FXII), prekallikrein (PK) and high-molecular weight kininogen. Fucosylated chondroitin sulfate (FCS) is a unique sulfated glycosaminoglycan (GAG) composed of a chondroitin sulfate-like backbone and sulfated fucose branches. The native FCS was preliminary found to cause undesired activation of the plasma contact system. How this unusual GAG functions in this process remains to be clarified. Herein, the relationship between its structure, plasma contact activation and its effects on the PK-FXII reciprocal activation loop were studied. The recalcification time assay indicated that the FCS at high concentration could be procoagulant which may be attributed to its contact activation activity. The structure-activity relationship study indicated that its high molecular weight and distinct fucose side chains are required for contact activation by FCS, although the sulfate substitution types of its side chains have less impact. In human plasma, the native FCSs potently induced FXII-dependent contact activation. However, in purified systems FCS did not significantly activate FXII per se or induce its autoactivation, whereas FCS significantly promoted the activation of PK by factor XIIa. Polysaccharide-protein interaction assays showed that FCS bound to PK with higher affinity than other contact system proteins. These data suggested that potent contact activation by FCS requires the positive feedback loop between PK and FXII. These findings contribute to better understanding of contact activation by complex GAG.

Published

2018

40. Peptidoglycan induces disseminated intravascular coagulation in baboons through activation of both coagulation pathways.

Author

Popescu NI, Silasi R, Keshari RS, Girton A, Burgett T, Zeerleder SS, Gailani D, Gruber A, Lupu F, and Coggeshall KM

Subjects

Animals, Anthrax pathology, Disseminated Intravascular Coagulation chemically induced, Disseminated Intravascular Coagulation pathology, Factor XIIa metabolism, Female, Male, Monocytes pathology, Papio, Papio anubis, Prekallikrein metabolism, Anthrax metabolism, Bacillus anthracis, Blood Coagulation drug effects, Disseminated Intravascular Coagulation blood, Monocytes metabolism

Abstract

Anthrax infections exhibit progressive coagulopathies that may contribute to the sepsis pathophysiology observed in fulminant disease. The hemostatic imbalance is recapitulated in primate models of late-stage disease but is uncommon in toxemic models, suggesting contribution of other bacterial pathogen-associated molecular patterns (PAMPs). Peptidoglycan (PGN) is a bacterial PAMP that engages cellular components at the cross talk between innate immunity and hemostasis. We hypothesized that PGN is critical for anthrax-induced coagulopathies and investigated the activation of blood coagulation in response to a sterile PGN infusion in primates. The PGN challenge, like the vegetative bacteria, induced a sepsis-like pathophysiology characterized by systemic inflammation, disseminated intravascular coagulation (DIC), organ dysfunction, and impaired survival. Importantly, the hemostatic impairment occurred early and in parallel with the inflammatory response, suggesting direct engagement of coagulation pathways. PGN infusion in baboons promoted early activation of contact factors evidenced by elevated protease-serpin complexes. Despite binding to contact factors, PGN did not directly activate either factor XII (FXII) or prekallikrein. PGN supported contact coagulation by enhancing enzymatic function of active FXII (FXIIa) and depressing its inhibition by antithrombin. In parallel, PGN induced de novo monocyte tissue factor expression in vitro and in vivo, promoting extrinsic clotting reactions at later stages. Activation of platelets further amplified the procoagulant state during PGN challenge, leading to DIC and subsequent ischemic damage of peripheral tissues. These data indicate that PGN may be a major cause for the pathophysiologic progression of Bacillus anthracis sepsis and is the primary PAMP behind the pathogen-induced coagulopathy in late-stage anthrax., (© 2018 by The American Society of Hematology.)

Published

2018

41. Factor XII Activation Promotes Platelet Consumption in the Presence of Bacterial-Type Long-Chain Polyphosphate In Vitro and In Vivo.

Author

Zilberman-Rudenko J, Reitsma SE, Puy C, Rigg RA, Smith SA, Tucker EI, Silasi R, Merkulova A, McCrae KR, Maas C, Urbanus RT, Gailani D, Morrissey JH, Gruber A, Lupu F, Schmaier AH, and McCarty OJT

Subjects

Animals, Blood Platelets metabolism, Disease Models, Animal, Factor XII genetics, Factor XIIa genetics, Female, Fibrin metabolism, Humans, Male, Mice, Inbred BALB C, Mice, Inbred C57BL, Mice, Knockout, Papio ursinus, Prekallikrein genetics, Prekallikrein metabolism, Pulmonary Embolism blood, Pulmonary Embolism chemically induced, Pulmonary Embolism genetics, Sepsis blood, Sepsis microbiology, Signal Transduction drug effects, Staphylococcal Infections blood, Staphylococcal Infections microbiology, Thrombosis blood, Thrombosis genetics, Tissue Kallikreins genetics, Tissue Kallikreins metabolism, Blood Coagulation drug effects, Blood Platelets drug effects, Factor XII metabolism, Factor XIIa metabolism, Platelet Activation drug effects, Polyphosphates toxicity, Thrombosis chemically induced

Abstract

Objective- Terminal complications of bacterial sepsis include development of disseminated intravascular consumptive coagulopathy. Bacterial constituents, including long-chain polyphosphates (polyP), have been shown to activate the contact pathway of coagulation in plasma. Recent work shows that activation of the contact pathway in flowing whole blood promotes thrombin generation and platelet activation and consumption distal to thrombus formation ex vivo and in vivo. Here, we sought to determine whether presence of long-chain polyP or bacteria in the bloodstream promotes platelet activation and consumption in a coagulation factor (F)XII-dependent manner. Approach and Results- Long-chain polyP promoted platelet P-selectin expression, microaggregate formation, and platelet consumption in flowing whole blood in a contact activation pathway-dependent manner. Moreover, long-chain polyP promoted local fibrin formation on collagen under shear flow in a FXI-dependent manner. Distal to the site of thrombus formation, platelet consumption was dramatically enhanced in the presence of long-chain polyP in the blood flow in a FXI- and FXII-dependent manner. In a murine model, long-chain polyP promoted platelet deposition and fibrin generation in lungs in a FXII-dependent manner. In a nonhuman primate model of bacterial sepsis, pre-treatment of animals with an antibody blocking FXI activation by FXIIa reduced lethal dose 100 Staphylococcus aureus-induced platelet and fibrinogen consumption. Conclusions- This study demonstrates that bacterial-type long-chain polyP promotes platelet activation in a FXII-dependent manner in flowing blood, which may contribute to sepsis-associated thrombotic processes, consumptive coagulopathy, and thrombocytopenia.

Published

2018

42. A structure-function analysis in patients with prekallikrein deficiency.

Author

Girolami A, Ferrari S, Cosi E, and Lombardi AM

Subjects

Adolescent, Adult, Aged, Amino Acid Sequence, Blood Coagulation Disorders complications, Blood Coagulation Disorders diagnosis, Blood Coagulation Disorders metabolism, Cardiovascular Diseases etiology, Cardiovascular Diseases physiopathology, Female, Genotype, Humans, Hypertension etiology, Hypertension physiopathology, Male, Middle Aged, Mutation, Prekallikrein metabolism, Structure-Activity Relationship, Young Adult, Blood Coagulation Disorders genetics, Prekallikrein chemistry, Prekallikrein deficiency, Prekallikrein genetics

Abstract

Objective: To investigate the structure-function relation in prekallikrein (PK) deficiency. PK is one of the proteins of the contact phase of blood coagulation which at the present time is the object of a revival of interest., Methods: All patients with PK deficiency who had been investigated by molecular biology techniques are the object of the present investigation. Details of patients were obtained from personal files and a time-unlimited PubMed search. Only cases with a molecular-biology-based diagnosis were included., Results: Twelve families were included. The total number of missense mutation was 10, together with 3 stop codons and 2 insertions. These mutations involved mainly exons 11 and 14. There were eight proved homozygotes and three compound heterozygotes. In one instance, homozygosity was probable but not proved. In nine cases, the defect was Type I, whereas it was Type II in the remaining three. No bleeding manifestations were present in 11 of the 12 probands. One proband had epistaxis, but she had hypertension. Altogether, four patients had hypertension and one of them had also two myocardial infarctions., Conclusions: Despite the paucity of cases, it was established that the majority of mutations involved the catalytic domain. It is auspicable that future reports of patients with this disorder should include molecular studies. This would certainly contribute to the understanding of the contact phase of blood coagulation.

Published

2018

43. The Plasma Kallikrein-Kininogen Pathway Is Critical in the Pathogenesis of Colitis in Mice.

Author

Wang B, Yang A, Zhao Z, He C, Liu Y, Colman RW, Dai J, and Wu Y

Subjects

Animals, Bradykinin blood, Colitis chemically induced, Dextran Sulfate, Factor XII metabolism, Interleukin-1beta analysis, Intestinal Mucosa pathology, Kininogen, High-Molecular-Weight genetics, Mice, Mice, Inbred C57BL, Mice, Knockout, Neutrophil Infiltration genetics, Neutrophils immunology, Plasma Kallikrein analysis, Prekallikrein genetics, Receptors, Bradykinin genetics, Trinitrobenzenesulfonic Acid, Bradykinin metabolism, Colitis immunology, Colitis pathology, Kallikrein-Kinin System immunology, Kininogen, High-Molecular-Weight metabolism, Prekallikrein metabolism

Abstract

The kallikrein-kinin system (KKS) consists of two serine proteases, prekallikrein (pKal) and factor XII (FXII), and a cofactor, high-molecular-weight kininogen (HK). Upon activation of the KKS, HK is cleaved to release bradykinin. Although the KKS is activated in humans and animals with inflammatory bowel disease (IBD), its role in the pathogenesis of IBD has not been characterized. In the present study, we determined the role of the KKS in the pathogenesis of IBD using mice that lack proteins involved in the KKS. In two colitis models, induced by dextran sulfate sodium (DSS) or 2,4,6-trinitrobenzene sulfonic acid (TNBS), mice deficient in HK, pKal, or bradykinin receptors displayed attenuated phenotypes, including body weight loss, disease activity index, colon length shortening, histological scoring, and colonic production of cytokines. Infiltration of neutrophils and inflammatory monocytes in the colonic lamina propria was reduced in HK-deficient mice. Reconstitution of HK-deficient mice through intravenous injection of HK recovered their susceptibility to DSS-induced colitis, increased IL-1β levels in the colon tissue and bradykinin concentrations in plasma. In contrast to the phenotypes of other mice lacking other proteins involved in the KKS, mice lacking FXII had comparable colonic inflammation to that observed in wild-type mice. The concentration of bradykinin was significantly increased in the plasma of wild-type mice after DSS-induced colitis. In vitro analysis revealed that DSS-induced pKal activation, HK cleavage, and bradykinin plasma release were prevented by the absence of pKal or the inhibition of Kal. Unlike DSS, TNBS-induced colitis did not trigger HK cleavage. Collectively, our data strongly suggest that Kal, acting independently of FXII, contributes to experimental colitis by promoting bradykinin release from HK.

Published

2018

44. Protocols to Assess Coagulation Following In Vitro Infection with Hemorrhagic Fever Viruses.

Author

Tursiella ML, Taylor SL, and Schmaljohn CS

Subjects

Bradykinin metabolism, Factor XII metabolism, Human Umbilical Vein Endothelial Cells, Humans, Kininogens metabolism, Prekallikrein metabolism, Thromboplastin metabolism, Hemorrhagic Fever with Renal Syndrome metabolism

Abstract

During the course of infection with a hemorrhagic fever virus (HFV), the checks and balances associated with normal coagulation are perturbed resulting in hemorrhage in severe cases and, in some patients, disseminated intravascular coagulopathy (DIC). While many HFVs have animal models that permit the analyses of systemic coagulopathy, animal infection models do not exist for all HFVs and moreover do not always recapitulate the pathology observed in human tissues. Furthermore, molecular analyses of how coagulation is affected are not always straightforward or practical when using ex-vivo animal-derived samples, thus reinforcing the importance of cell culture studies. This chapter highlights procedures utilizing human umbilical vein endothelial cells (HUVECs) as a model system to evaluate components of the intrinsic (prekallikrein (PK), factor XII (FXII), kininogen, and bradykinin (BK)) and extrinsic (Tissue Factor (TF)) systems. Specifically, protocols are included for the generation of a coculture blood vessel model, plating and infection of HUVEC monolayers and assays designed to measure activation of PK and FXII, cleavage of kininogen, and to measure the expression of TF mRNA and protein.

Published

2018

45. Streptococcus gallolyticus subsp. gallolyticus endocarditis isolate interferes with coagulation and activates the contact system.

Author

Isenring J, Köhler J, Nakata M, Frank M, Jans C, Renault P, Danne C, Dramsi S, Kreikemeyer B, and Oehmcke-Hecht S

Subjects

Bacterial Proteins metabolism, Factor XII metabolism, Fimbriae, Bacterial genetics, Kininogen, High-Molecular-Weight metabolism, Prekallikrein metabolism, Protein Binding, Streptococcus gallolyticus subspecies gallolyticus genetics, Streptococcus gallolyticus subspecies gallolyticus growth & development, Virulence, Virulence Factors genetics, Blood Coagulation, Blood Coagulation Factors metabolism, Fimbriae, Bacterial metabolism, Streptococcal Infections metabolism, Streptococcus gallolyticus subspecies gallolyticus pathogenicity, Virulence Factors metabolism

Abstract

Streptococcus gallolyticus subsp. gallolyticus, formerly classified as S. bovis biotype I, is an increasing cause of bacteremia and infective endocarditis in the elderly. The physiopathology of infective endocarditis is poorly understood and involves immune and coagulation systems. In this study, we found that S. gallolyticus subsp. gallolyticus activates the human contact system, which in turn has two consequences: cleavage of high-molecular-weight kininogen (HK) resulting in release of the potent pro-inflammatory peptide bradykinin, and initiation of the intrinsic pathway of coagulation. S. gallolyticus subsp. gallolyticus was found to bind and activate factors of the human contact system at its surface, leading to a significant prolongation of the intrinsic coagulation time and to the release of bradykinin. High-affinity binding of factor XII to the bacterial Pil1 collagen binding protein was demonstrated with a K D of 13 nM. Of note, Pil1 expression was exclusively found in S. gallolyticus subsp. gallolyticus, further supporting an essential contribution of this pilus in virulence.

Published

2018

46. A kallikrein-targeting RNA aptamer inhibits the intrinsic pathway of coagulation and reduces bradykinin release.

Author

Steen Burrell KA, Layzer J, and Sullenger BA

Subjects

Anticoagulants metabolism, Aptamers, Nucleotide genetics, Aptamers, Nucleotide metabolism, Dose-Response Relationship, Drug, Factor XIIa metabolism, Humans, Kallikreins genetics, Kinetics, Kininogen, High-Molecular-Weight metabolism, Partial Thromboplastin Time, Prekallikrein metabolism, Protein Binding, Thrombosis blood, Thrombosis genetics, Anticoagulants pharmacology, Aptamers, Nucleotide pharmacology, Blood Coagulation drug effects, Bradykinin metabolism, Kallikreins metabolism, Thrombosis prevention & control

Abstract

Essentials Kallikrein amplifies contact activation and is a potential target for preventing thrombosis. We developed and characterized a kallikrein aptamer using convergent evolution and kinetic assays. Kall1-T4 prolongs intrinsic clotting time by inhibiting factor XIIa-mediated prekallikrein activation. Kall1-T4 decreases high-molecular-weight kininogen cleavage and bradykinin release., Summary: Background Plasma kallikrein is a serine protease that plays an integral role in many biological processes, including coagulation, inflammation, and fibrinolysis. The main function of kallikrein in coagulation is the amplification of activated factor XII (FXIIa) production, which ultimately leads to thrombin generation and fibrin clot formation. Kallikrein is generated by FXIIa-mediated cleavage of the zymogen prekallikrein, which is usually complexed with the non-enzymatic cofactor high molecular weight kininogen (HK). HK also serves as a substrate for kallikrein to generate the proinflammatory peptide bradykinin (BK). Interestingly, prekallikrein-deficient mice are protected from thrombotic events while retaining normal hemostatic capacity. Therefore, therapeutic targeting of kallikrein may provide a safer alternative to traditional anticoagulants with anti-inflammatory benefits. Objectives To isolate and characterize an RNA aptamer that binds to and inhibits plasma kallikrein, and to elucidate its mechanism of action. Methods and Results Using convergent Systematic Evolution of Ligands by Exponential Enrichment (SELEX), we isolated an RNA aptamer that targets kallikrein. This aptamer, Kall1-T4, specifically binds to both prekallikrein and kallikrein with similar subnanomolar binding affinities, and dose-dependently prolongs fibrin clot formation in an activated partial thromboplastin time (APTT) coagulation assay. In a purified in vitro system, Kall1-T4 inhibits the reciprocal activation of prekallikrein and FXII primarily by reducing the rate of FXIIa-mediated prekallikrein activation. Additionally, Kall1-T4 significantly reduces kallikrein-mediated HK cleavage and subsequent BK release. Conclusions We have isolated a specific and potent inhibitor of prekallikrein/kallikrein activity that serves as a powerful tool for further elucidating the role of kallikrein in thrombosis and inflammation., (© 2017 International Society on Thrombosis and Haemostasis.)

Published

2017

47. Single-chain factor XII: a new form of activated factor XII.

Author

Ivanov I, Matafonov A, and Gailani D

Subjects

Factor XIIa genetics, Humans, Plasma Kallikrein genetics, Prekallikrein genetics, Recombinant Proteins genetics, Recombinant Proteins metabolism, Factor XIIa metabolism, Plasma Kallikrein metabolism, Prekallikrein metabolism

Abstract

Purpose of Review: Exposure of blood to foreign surfaces induces reciprocal conversion of the plasma proteins factor XII (fXII) and plasma prekallikrein (PPK) to the proteases α-fXIIa and α-kallikrein. This process, called contact activation, has a range of effects on host defence mechanisms, including promoting coagulation. The nature of the triggering mechanism for contact activation is debated. One hypothesis predicts that fXII has protease activity, either intrinsically or upon surface-binding, that initiates contact activation. We tested this by assessing the proteolytic activity of a recombinant fXII variant that cannot be converted to α-fXIIa., Recent Findings: The proteolytic activity of fXII-T (for 'triple' mutant), a variant with alanine substitutions for arginine at activation cleavage sites (Arg334, Arg344, and Arg353) was tested with known α-fXIIa substrates. FXII-T activates PPK in solution, and the reaction is enhanced by polyphosphate, an inducer of contact activation released from platelets. In the presence of polyphosphate, fXII-T converts fXII to α-fXIIa, and also converts the coagulation protein factor XI to its active form., Summary: The findings support the hypothesis that contact activation is initiated through activity intrinsic to single-chain fXII, and indicate that preexisting α-fXIIa is not required for induction of contact activation.

Published

2017

48. Cytokine and estrogen stimulation of endothelial cells augments activation of the prekallikrein-high molecular weight kininogen complex: Implications for hereditary angioedema.

Author

Joseph K, Tholanikunnel BG, and Kaplan AP

Subjects

Angioedemas, Hereditary metabolism, Cells, Cultured, Factor XII metabolism, HSP90 Heat-Shock Proteins metabolism, Human Umbilical Vein Endothelial Cells metabolism, Humans, Tissue Plasminogen Activator metabolism, Urokinase-Type Plasminogen Activator metabolism, Estradiol pharmacology, Estrogens pharmacology, Human Umbilical Vein Endothelial Cells drug effects, Interleukin-1 pharmacology, Kininogen, High-Molecular-Weight metabolism, Prekallikrein metabolism, Tumor Necrosis Factor-alpha pharmacology

Abstract

Background: When the prekallikrein-high molecular weight kininogen complex is bound to endothelial cells, prekallikrein is stoichiometrically converted to kallikrein because of release of heat shock protein-90 (Hsp90). Although bradykinin formation is typically initiated by factor XII autoactivation, it is also possible to activate factor XII either by kallikrein, thus formed, or by plasmin., Objective: Because attacks of hereditary angioedema can be related to infection and/or exposure to estrogen, we questioned whether estrogen or cytokine stimulation of endothelial cells could augment release of Hsp90 and prekallikrein activation. We also tested release of profibrinolytic enzymes, urokinase, and tissue plasminogen activator (TPA) as a source for plasmin formation., Methods: Cells were stimulated with agonists, and secretion of Hsp90, urokinase, and TPA was measured in the culture supernatants by ELISA. Activation of the prekallikrein-HK complex was measured by using pro-phe-arg-p-nitroanilide reflecting kallikrein formation., Results: Hsp90 release was stimulated with optimal doses of estradiol, IL-1, and TNF-α (10 ng/mL) from 15 minutes to 120 minutes. TPA release was not augmented by any of the agonists tested but urokinase was released by IL-1, TNF-α, and thrombin (positive control), but not estrogen. Augmented activation of the prekallikrein-HK complex to generate kallikrein was seen with each agonist that releases Hsp90. Addition of 0.1% factor XII relative to prekallikrein-HK leads to rapid formation of kallikrein; factor XII alone does not autoactivate., Conclusions: IL-1, TNF-α, and estrogen stimulate release of Hsp90 and augment activation of the prekallikrein-HK complex to generate kallikrein and bradykinin. IL-1 and TNF-α stimulate release of urokinase, which can convert plasminogen to plasmin and represents a possible source for plasmin generation in all types of hereditary angioedema, but particularly hereditary angioedema with normal C1 inhibitor with a factor XII mutation. Both kallikrein and plasmin activate factor XII; kallikrein is 20 times more potent on a molar basis., (Copyright © 2016 American Academy of Allergy, Asthma & Immunology. Published by Elsevier Inc. All rights reserved.)

Published

2017

49. Nucleic acids as cofactors for factor XI and prekallikrein activation: Different roles for high-molecular-weight kininogen.

Author

Ivanov I, Shakhawat R, Sun MF, Dickeson SK, Puy C, McCarty OJ, Gruber A, Matafonov A, and Gailani D

Subjects

Enzyme Activation, Factor XIIa metabolism, Humans, Thrombin metabolism, Time Factors, Blood Coagulation, DNA metabolism, Factor XIa metabolism, Kininogen, High-Molecular-Weight metabolism, Prekallikrein metabolism, RNA metabolism

Abstract

The plasma zymogens factor XI (fXI) and prekallikrein (PK) are activated by factor XIIa (fXIIa) during contact activation. Polyanions such as DNA and RNA may contribute to thrombosis and inflammation partly by enhancing PK and fXI activation. We examined PK and fXI activation in the presence of nucleic acids, and determine the effects of the cofactor high molecular weight kininogen (HK) on the reactions. In the absence of HK, DNA and RNA induced fXI autoactivation. Proteases known to activate fXI (fXIIa and thrombin) did not enhance this process appreciably. Nucleic acids had little effect on PK activation by fXIIa in the absence of HK. HK had significant but opposite effects on PK and fXI activation. HK enhanced fXIIa activation of PK in the presence of nucleic acids, but blocked fXI autoactivation. Thrombin and fXIIa could overcome the HK inhibitory effect on autoactivation, indicating these proteases are necessary for nucleic acid-induced fXI activation in an HK-rich environment such as plasma. In contrast to PK, which requires HK for optimal activation, fXI activation in the presence of nucleic acids depends on anion binding sites on the fXI molecule. The corresponding sites on PK are not necessary for PK activation. Our results indicate that HK functions as a cofactor for PK activation in the presence of nucleic acids in a manner consistent with classic models of contact activation. However, HK has, on balance, an inhibitory effect on nucleic acid-supported fXI activation and may function as a negative regulator of fXI activation.

Published

2017

50. Complement, Kinins, and Hereditary Angioedema: Mechanisms of Plasma Instability when C1 Inhibitor is Absent.

Author

Kaplan AP and Joseph K

Subjects

Angioedemas, Hereditary diagnosis, Bradykinin metabolism, Complement Activation immunology, Complement C1 Inhibitor Protein genetics, Complement C1 Inhibitor Protein metabolism, Complement System Proteins metabolism, Enzyme Activation, Factor XII metabolism, Hereditary Angioedema Types I and II diagnosis, Hereditary Angioedema Types I and II etiology, Hereditary Angioedema Types I and II metabolism, Humans, Kininogen, High-Molecular-Weight metabolism, Prekallikrein metabolism, Protein Binding, Angioedemas, Hereditary etiology, Angioedemas, Hereditary metabolism, Complement System Proteins immunology, Kinins metabolism

Abstract

Plasma of patients with types I and II hereditary angioedema is unstable if incubated in a plastic (i.e., inert) vessel at 37 °C manifested by progressively increasing formation of bradykinin. There is also a persistent low level of C4 in 95 % of patients even when they are symptomatic. These phenomena are due to the properties of the C1r subcomponent of C1, factor XII, and the bimolecular complex of prekallikrein with high molecular weight kininogen (HK). Purified C1r auto-activates in physiologic buffers, activates C1s, which in turn depletes C4. This occurs when C1 inhibitor is deficient. The complex of prekallikrein-HK acquires an inducible active site not present in prekallikrein which in Tris-type buffers cleaves HK stoichiometrically to release bradykinin, or in phosphate buffer auto-activates to generate kallikrein and bradykinin. Thus immunologic depletion of C1 inhibitor from factor XII-deficient plasma (phosphate is the natural buffer) auto-activates on incubation to release bradykinin. Normal C1 inhibitor prevents this from occurring. During attacks of angioedema, if factor XII auto-activates on surfaces, the initial factor XIIa formed converts prekallikrein to kallikrein, and kallikrein cleaves HK to release bradykinin. Kallikrein also rapidly activates most remaining factor XII to factor XIIa. Additional cleavages convert factor XIIa to factor XIIf and factor XIIf activates C1r enzymatically so that C4 levels approach zero, and C2 is depleted. There is also a possibility that kallikrein is generated first as a result of activation of the prekallikrein-HK complex by heat shock protein 90 released from endothelial cells, followed by kallikrein activation of factor XII.

Published

2016