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.
Subject(s)
Blood Coagulation/physiology , Complement C1 Inhibitor Protein/metabolism , Factor XII/metabolism , Hereditary Angioedema Type III/immunology , Hereditary Angioedema Type III/pathology , Prekallikrein/metabolism , 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 AdultABSTRACT
The plasma proteins factor XII (FXII) and prekallikrein (PK) undergo reciprocal activation to the proteases FXIIa and kallikrein by a process that is enhanced by surfaces (contact activation) and regulated by the serpin C1 inhibitor. Kallikrein cleaves high-molecular-weight kininogen (HK), releasing the vasoactive peptide bradykinin. Patients with hereditary angioedema (HAE) experience episodes of soft tissue swelling as a consequence of unregulated kallikrein activity or increased prekallikrein activation. Although most HAE cases are caused by reduced plasma C1-inhibitor activity, HAE has been linked to lysine/arginine substitutions for Thr309 in FXII (FXII-Lys/Arg309). Here, we show that FXII-Lys/Arg309 is susceptible to cleavage after residue 309 by coagulation proteases (thrombin and FXIa), resulting in generation of a truncated form of FXII (δFXII). The catalytic efficiency of δFXII activation by kallikrein is 15-fold greater than for full-length FXII. The enhanced rate of reciprocal activation of PK and δFXII in human plasma and in mice appears to overwhelm the normal inhibitory function of C1 inhibitor, leading to increased HK cleavage. In mice given human FXII-Lys/Arg309, induction of thrombin generation by infusion of tissue factor results in enhanced HK cleavage as a consequence of δFXII formation. The effects of δFXII in vitro and in vivo are reproduced when wild-type FXII is bound by an antibody to the FXII heavy chain (HC; 15H8). The results contribute to our understanding of the predisposition of patients carrying FXII-Lys/Arg309 to angioedema after trauma, and reveal a regulatory function for the FXII HC that normally limits PK activation in plasma.
Subject(s)
Factor XII/chemistry , Factor XIa/chemistry , Hereditary Angioedema Type III/blood , Hereditary Angioedema Type III/genetics , Angioedemas, Hereditary , Animals , Arginine/chemistry , Blood Coagulation , Bradykinin/blood , Catalysis , Complement C1 Inhibitor Protein/chemistry , Factor XIIa/chemistry , HEK293 Cells , Humans , Kininogens/blood , Lysine/chemistry , Mice , Mice, Inbred C57BL , Plasma Kallikrein/chemistry , Prekallikrein/chemistry , Protein Binding , Recombinant Proteins/chemistry , Surface Properties , Thrombin/geneticsABSTRACT
Contact activation is the surface-induced conversion of factor XII (FXII) zymogen to the serine protease FXIIa. Blood-circulating FXII binds to negatively charged surfaces and this contact to surfaces triggers a conformational change in the zymogen inducing autoactivation. Several surfaces that have the capacity for initiating FXII contact activation have been identified, including misfolded protein aggregates, collagen, nucleic acids, and platelet and microbial polyphosphate. Activated FXII initiates the proinflammatory kallikrein-kinin system and the intrinsic coagulation pathway, leading to formation of bradykinin and thrombin, respectively. FXII contact activation is well characterized in vitro and provides the mechanistic basis for the diagnostic clotting assay, activated partial thromboplastin time. However, only in the past decade has the critical role of FXII contact activation in pathological thrombosis been appreciated. While defective FXII contact activation provides thromboprotection, excess activation underlies the swelling disorder hereditary angioedema type III. This review provides an overview of the molecular basis of FXII contact activation and FXII contact activation-associated disease states.
Subject(s)
Blood Coagulation , Bradykinin/metabolism , Factor XIIa/metabolism , Hereditary Angioedema Type III/metabolism , Thrombin/metabolism , Animals , Bradykinin/genetics , Enzyme Activation , Factor XIIa/genetics , Hereditary Angioedema Type III/genetics , Humans , Thrombin/geneticsABSTRACT
Hereditary angioedema with normal C1 esterase inhibitor and mutations in the F12 gene (HAE-FXII) is associated with skin swellings, abdominal pain attacks, and the risk of asphyxiation due to upper airway obstruction. It occurs nearly exclusively in women. We report our experience treating HAE-FXII with discontinuation of potential trigger factors and drug therapies. The study included 72 patients with HAE-FXII. Potential triggers included estrogen-containing oral contraceptives (eOC), hormonal replacement therapy, or angiotensin-converting enzyme inhibitors. Drug treatment comprised plasma-derived C1 inhibitor (pdC1-INH) for acute swelling attacks and progestins, tranexamic acid, and danazol for the prevention of attacks. Discontinuation of eOC was effective in 25 (89.3%) of 28 women and led to a reduction in the number of attacks (about 90%). After ending hormonal replacement therapy, three of eight women became symptom-free. Three women with exacerbation of HAE-FXII during intake of quinapril or enalapril had no further HAE-FXII attacks after discontinuation of those drugs. Eleven women were treated with pdC1-INH for 143 facial attacks. The duration of the treated facial attacks (mean: 26.6 h; SD: 10.1 h) was significantly shorter than that of the previous 88 untreated facial attacks in the same women (mean: 64.1 h; SD: 28.0 h; P < 0.01). The mean reduction in attack frequency was 99.8% under progestins after discontinuing eOC (16 women), 93.8% under tranexamic acid (four women), and 100% under danazol (three women). For patients with HAE-FXII, various treatment options are available which completely or at least partially reduce the number or duration of attacks.
Subject(s)
Complement C1 Inhibitor Protein/therapeutic use , Hereditary Angioedema Type III/drug therapy , Adolescent , Adult , Aged , Angiotensin-Converting Enzyme Inhibitors/adverse effects , Biomarkers , Chemoprevention , Child , Disease Progression , Estrogens/adverse effects , Factor XII/genetics , Female , Hereditary Angioedema Type III/blood , Hereditary Angioedema Type III/diagnosis , Hereditary Angioedema Type III/genetics , Humans , Male , Middle Aged , Mutation , Risk Factors , Treatment Outcome , Young AdultSubject(s)
DNA Mutational Analysis , Factor XII/genetics , Genetic Testing/methods , Hereditary Angioedema Type III/genetics , Mutation , Adult , Female , Genetic Markers , Genetic Predisposition to Disease , Hereditary Angioedema Type III/blood , Hereditary Angioedema Type III/diagnosis , Hereditary Angioedema Type III/immunology , Hereditary Angioedema Type III/therapy , Humans , Phenotype , Predictive Value of Tests , Risk Factors , Tomography, X-Ray ComputedABSTRACT
Hereditary angioedema type III (HAEIII) is a rare inherited swelling disorder that is associated with point mutations in the gene encoding the plasma protease factor XII (FXII). Here, we demonstrate that HAEIII-associated mutant FXII, derived either from HAEIII patients or recombinantly produced, is defective in mucin-type Thr309-linked glycosylation. Loss of glycosylation led to increased contact-mediated autoactivation of zymogen FXII, resulting in excessive activation of the bradykinin-forming kallikrein-kinin pathway. In contrast, both FXII-driven coagulation and the ability of C1-esterase inhibitor to bind and inhibit activated FXII were not affected by the mutation. Intravital laser-scanning microscopy revealed that, compared with control animals, both F12-/- mice reconstituted with recombinant mutant forms of FXII and humanized HAEIII mouse models with inducible liver-specific expression of Thr309Lys-mutated FXII exhibited increased contact-driven microvascular leakage. An FXII-neutralizing antibody abolished bradykinin generation in HAEIII patient plasma and blunted edema in HAEIII mice. Together, the results of this study characterize the mechanism of HAEIII and establish FXII inhibition as a potential therapeutic strategy to interfere with excessive vascular leakage in HAEIII and potentially alleviate edema due to other causes.
Subject(s)
Blood Coagulation , Factor XII/metabolism , Hereditary Angioedema Type III/metabolism , Mutation, Missense , Adult , Amino Acid Substitution , Animals , Antibodies, Neutralizing/pharmacology , Bradykinin/genetics , Bradykinin/metabolism , Disease Models, Animal , Factor XII/genetics , Female , Glycosylation/drug effects , Hereditary Angioedema Type III/drug therapy , Hereditary Angioedema Type III/genetics , Hereditary Angioedema Type III/pathology , Humans , Mice , Mice, KnockoutABSTRACT
Combinations of proinflammatory and procoagulant reactions are the unifying principle for a variety of disorders affecting the cardiovascular system. Factor XII (FXII, Hageman factor) is a plasma protease that initiates the contact system. The biochemistry of the contact system in vitro is well understood; however, its in vivo functions are just beginning to emerge. The current review concentrates on activators and functions of the FXII-driven contact system in vivo. Elucidating its physiologic activities offers the exciting opportunity to develop strategies for the safe interference with both thrombotic and inflammatory diseases.
Subject(s)
Factor XII/physiology , Animals , Blood Coagulation/physiology , Enzyme Activation , Factor XII/genetics , Factor XII Deficiency/blood , Factor XII Deficiency/genetics , Heparin/pharmacology , Hereditary Angioedema Type III/blood , Hereditary Angioedema Type III/genetics , Humans , Mice , Models, Animal , Models, Biological , Platelet Activation , Polyphosphates/blood , Protein Aggregates , Risk , Thrombosis/blood , Thrombosis/epidemiologyABSTRACT
In this article, three cases of hereditary angioedema (HAE) type III (estrogen-dependent or with normal C1 inhibitor) are reported. The HAE was initially described in women of the same family in association with high-leveled estrogenic conditions such as the use of oral contraceptives and pregnancy. There is no change in the C1 inhibitor as happens in other types of hereditary angioedema, and mutations are observed in the encoding gene of the XII factor of coagulation in several patients. The current diagnosis is mainly clinical and treatment consists in the suspension of the triggering factors and control of acute symptoms. A brief review of physiopathology, clinical features, genetic alterations and treatment are also presented.
Subject(s)
Hereditary Angioedema Type III/genetics , Adult , Complement C1 Inhibitor Protein/metabolism , Estrogens/metabolism , Female , Hereditary Angioedema Type III/diagnosis , Hereditary Angioedema Type III/therapy , Humans , Lip , Mutation , Treatment OutcomeABSTRACT
In this article, three cases of hereditary angioedema (HAE) type III (estrogen-dependent or with normal C1 inhibitor) are reported. The HAE was initially described in women of the same family in association with high-leveled estrogenic conditions such as the use of oral contraceptives and pregnancy. There is no change in the C1 inhibitor as happens in other types of hereditary angioedema, and mutations are observed in the encoding gene of the XII factor of coagulation in several patients. The current diagnosis is mainly clinical and treatment consists in the suspension of the triggering factors and control of acute symptoms. A brief review of physiopathology, clinical features, genetic alterations and treatment are also presented.
Neste artigo são relatados três casos de angioedema hereditário do tipo III (estrógeno-dependente ou com inibidor de C1 normal), que foi inicialmente descrito em mulheres da mesma família, em associação com condições de alto nível estrogênico, como uso de anticoncepcionais orais e gravidez. Não há alteração do inibidor de C1, como acontece nos outros tipos de angioedema hereditário, e são observadas mutações no gene codificador do fator XII da coagulação em várias pacientes. O diagnóstico atualmente é eminentemente clínico e o tratamento consiste na suspensão dos fatores desencadeantes e controle dos sintomas agudos. Também é apresentada breve revisão da fisiopatogenia, quadro clínico, alterações genéticas e tratamento.
Subject(s)
Adult , Female , Humans , Hereditary Angioedema Type III/genetics , Complement C1 Inhibitor Protein/metabolism , Estrogens/metabolism , Hereditary Angioedema Type III/diagnosis , Hereditary Angioedema Type III/therapy , Lip , Mutation , Treatment OutcomeSubject(s)
Angioedemas, Hereditary/genetics , Angioedemas, Hereditary/physiopathology , Factor XII/genetics , Hereditary Angioedema Type III/genetics , Mutation , Adolescent , Adult , Factor XII/chemistry , Family , Female , Humans , Lysine/genetics , Male , Pedigree , Severity of Illness Index , Spain , Threonine/genetics , Young AdultABSTRACT
BACKGROUND: A new variant of hereditary angioedema has been reported during the last decade. Three main characteristics distinguish it from classic hereditary angioedema: normal C1 inhibitor activity, predominance in women, and different genetic alterations. OBJECTIVE: To assess the symptoms, laboratory findings, and treatment of a population with type III hereditary angioedema from Northwest Spain. METHODS: We studied 29 patients (26 female and 3 male) from 13 different families. RESULTS: The 26 female patients showed a similar clinical pattern to the classic forms of hereditary angioedema, and 22 of these patients had the estrogen-dependent phenotype. Three patients had a negative family history, and 1 of the parents was confirmed as an asymptomatic carrier in 2 of them. All had functional C1 inhibitor activity within the normal range in periods without high estrogen levels, but during attacks (in female patients) and pregnancy, activity decreased to below 50%. One male patient had normal C1 inhibitor activity during attacks, and he was initially diagnosed as having idiopathic angioedema. The C4 and antigenic C1 inhibitor levels were always normal. All studied patients had the c.1032C>A, Thr309Lys mutation in the factor XII gene. The mutation was also found in asymptomatic relatives: 5 of 6 men studied and 1 of 8 women studied. CONCLUSION: Positive family history is a diagnosis criterion, but it could be lacking because there may be asymptomatic relatives, primarily males.
