Enzymatic Assays for the Diagnosis of Bradykinin-Dependent Angioedema

Defendi, Federica; Charignon, Delphine; Ghannam, Arije; Baroso, Rémi; Csopaki, Françoise; Allegret-Cadet, Marion; Ponard, D.; Favier, Bertrand; Cichon, Sven; Nicolie, Brigitte; Fain, Olivier; Martin, Ludovic; Drouet, Christian

doi:10.1371/journal.pone.0070140

Cited by 59 publications

(67 citation statements)

References 29 publications

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“…However, the existence of both acquired (idiopathic non-histaminergic AAO - InH-AAO) and hereditary (HAO of unknown origin - U-HAO) has been acknowledged in the most recent classification of AO under the patronage of the European Academy of Allergy and Clinical Immunology [10]. From our side, we demonstrated that some of these AOs could be related to an increased kinin formation and/or to a decreased BK catabolism associated with a deficiency in one or several kininase(s) [15,22,23,24]. …”

Section: Introductionmentioning

confidence: 72%

“…C1-INH analysis included quantitative and functional measurements [30]. Kinin formation was evaluated by measurement of the plasma spontaneous amidase activity using the HD-Pro-Phe-Arg- p NA substrate as recently described [24]. This assay evaluates the activity of the enzymes responsible for BK production after cleaving high-molecular weight kininogen, the serine proteases of contact phase (kallikrein, FXII).…”

Section: Methodsmentioning

confidence: 99%

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Distinct Conditions Support a Novel Classification for Bradykinin-Mediated Angio-Oedema

Dessart

Defendi²,

Humeau³

et al. 2015

Dermatology

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Background: Angio-oedema (AO) can be attributable to bradykinin (BK) accumulation, as is the case for prototypical hereditary AO (HAO) due to C1 inhibitor (C1-INH) deficiency. However, our clinical experience in a reference centre has shown that some patients display a clinical history suggestive of HAO, but exhibit normal C1-INH function, have no mutation in the causative genes associated with HAO (SERPING1, F12), and report no intake of drugs known to promote AO. Objective: We sought to determine the frequency and distribution of different AO subtypes suspected to be BK-mediated AO (BK-AO) and defined by clinical, history and biological criteria (enzyme activities implicated in BK formation and catabolism). Methods: The files of all patients referred to our centre for suspected BK-AO were retrospectively analysed. Results: The distribution of patients (n = 162) was 16 and 4% with a hereditary deficiency of C1-INH or a gain of factor XII function, respectively, 29% with iatrogenic BK-AO, 21% with non-iatrogenic defective kininase activity and 30% with idiopathic increased kinin formation. Conclusion: BK-AO may be caused by multiple inherited or acquired factors triggering BK accumulation. Therefore, we propose a novel typology for BK-AO based on the imbalance of production/catabolism of BK.

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Section: Introductionmentioning

confidence: 72%

Section: Methodsmentioning

confidence: 99%

Distinct Conditions Support a Novel Classification for Bradykinin-Mediated Angio-Oedema

Dessart

Defendi²,

Humeau³

et al. 2015

Dermatology

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“…Conceptually, given the fact that these mutations affect the prolin-rich domain of FXII, which is considered to play a role in the interaction with negatively charged surfaces, one might speculate that these forms of FXII are more prone to activation upon contact with negatively charged surfaces (58). Spontaneous amidase activity in plasma as a surrogate marker for serine protease activity of the CP and fibrinolytic system has been shown to be increased in patients with FXII-HAE regardless the clinical severity (60). Interestingly, ACE and CPN activity levels inversely correlated with disease severity pointing to the important role of BKdegrading enzymes in the pathogenesis of HAE type III, but most probably in other forms as well (61).…”

Section: C1-inhibitor Regulates Bk Generationmentioning

confidence: 99%

“…Clotting factor-based assays may help to identify increased activity of FXIIa in plasma (57). In a collective of 100 symptomatic patients suffering from FXII-HAE spontaneous amidase activity (see above) has been shown to correlate with disease severity (60). However, specific genetic testing for the known FXII mutations or sequencing of the FXII gene is the most appropriate diagnostic tools to confirm or exclude HAE type III (9).…”

Section: Diagnosismentioning

confidence: 99%

Hereditary and acquired C1-inhibitor-dependent angioedema: from pathophysiology to treatment

Zeerleder

Levi

2016

Annals of Medicine

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Uncontrolled generation of bradykinin (BK) due to insufficient levels of protease inhibitors controlling contact phase (CP) activation, increased activity of CP proteins, and/or inadequate degradation of BK into inactive peptides increases vascular permeability via BK-receptor 2 (BKR2) and results in subcutaneous and submucosal edema formation. Hereditary and acquired angioedema due to C1-inhibitor deficiency (C1-INH-HAE and -AAE) are diseases characterized by serious and potentially fatal attacks of subcutaneous and submucosal edemas of upper airways, facial structures, abdomen, and extremities, due to inadequate control of BK generation. A decreased activity of C1-inhibitor is the hallmark of C1-INH-HAE (types 1 and 2) due to a mutation in the C1-inhibitor gene, whereas the deficiency in C1-inhibitor in C1-INH-AAE is the result of autoimmune phenomena. In HAE with normal C1-inhibitor, a significant percentage of patients have an increased activity of factor XIIa due to a FXII mutation (FXII-HAE). Treatment of C1-inhibitordependent angioedema focuses on restoring control of BK generation by inhibition of CP proteases by correcting the balance between CP inhibitors and BK breakdown or by inhibition of BK-mediated effects at the BKR2 on endothelial cells. This review will address the pathophysiology, clinical picture, diagnosis and available treatment in C1-inhibitor-dependent angioedema focusing on BK-release and its regulation. ä KEY MESSAGESInadequate control of bradykinin formation results in the formation of characteristic subcutaneous and submucosal edemas of the skin, upper airways, facial structures, abdomen and extremities as seen in hereditary and acquired C1-inhibitor-dependent angioedema. Diagnosis of hereditary and acquired C1-inhibitor-dependent angioedema may be troublesome as illustrated by the fact that there is a significant delay in diagnosis; a certain grade of suspicion is therefore crucial for quick diagnosis. Submucosal edema formation in hereditary and acquired C1-inhibitor-dependent angioedema is potentially life threatening and can occur at any age. To date effective therapies for acute and prophylactic treatment are available. ARTICLE HISTORY

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“…The therapeutic response to specific antagonists characterizes IH-AAE. Bradykinin mediates ACEI-AAE and C1-INH-HAE, and possibly also FXII-HAE, U-HAE and InH-AAE [12,13]. Leukotrienes, and other yet undefined factors, are likely to be involved in some cases of drug-related angioedema [1].…”

Section: Introductionmentioning

confidence: 99%

Presentation, diagnosis and treatment of angioedema without wheals: a retrospective analysis of a cohort of 1058 patients

et al. 2014

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Enzymatic Assays for the Diagnosis of Bradykinin-Dependent Angioedema

Cited by 59 publications

References 29 publications

Distinct Conditions Support a Novel Classification for Bradykinin-Mediated Angio-Oedema

Distinct Conditions Support a Novel Classification for Bradykinin-Mediated Angio-Oedema

Hereditary and acquired C1-inhibitor-dependent angioedema: from pathophysiology to treatment

Presentation, diagnosis and treatment of angioedema without wheals: a retrospective analysis of a cohort of 1058 patients

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