Your search keyword '"Kaplan AP"' showing total 392 results

51. Omalizumab substantially improves dermatology-related quality of life in patients with chronic spontaneous urticaria.

Author

Finlay AY, Kaplan AP, Beck LA, Antonova EN, Balp MM, Zazzali J, Khalil S, and Maurer M

Subjects

Adolescent, Adult, Aged, Child, Chronic Disease, Double-Blind Method, Female, Humans, Male, Middle Aged, Placebos, Urticaria physiopathology, Young Adult, Anti-Allergic Agents therapeutic use, Omalizumab therapeutic use, Quality of Life, Urticaria drug therapy

Abstract

Background: Chronic spontaneous/idiopathic urticaria (CSU/CIU) has substantial detrimental effects on health-related quality of life (HRQoL) with an effect comparable to or worse than many other skin diseases., Objective: To assess the effect of omalizumab on CSU patients' HRQoL, measured by the Dermatology Life Quality Index (DLQI) in three phase III studies ASTERIA I, ASTERIA II and GLACIAL., Methods: A post hoc analysis examined changes in DLQI scores, distribution of patients across DLQI bands and the proportion reaching minimal clinically important difference (MCID) following omalizumab vs. placebo., Results: Omalizumab 300 mg significantly improved total DLQI scores vs. placebo, with a mean decrease from baseline to week 12 of -10.3 vs. -6.1 (P < 0.0001) in ASTERIA I, -10.2 vs. -6.1 (P = 0.0004) in ASTERIA II and -9.7 vs. -5.1 (P < 0.0001) in GLACIAL. A significant shift from high disease impact on life at baseline towards less impact at week 12 was seen with omalizumab 300 mg vs. placebo (P < 0.001; all studies). The proportion of patients where change in mean total DLQI score from baseline to week 12 reached an MCID of ≥4 was 74.1%, 76.0% and 77.2% in ASTERIA I, II and GLACIAL, respectively (P < 0.01; all studies)., Limitations: Maximum duration of omalizumab treatment was 24 weeks., Conclusion: This additional analysis assessed the impact of CSU and benefit of treatment with omalizumab by exploring different facets of DLQI data by treatment arm at multiple assessment points. The original aspects of analysis included applying the concept of the recently validated score for the MCID of the DLQI, changes in DLQI domain scores and in the distribution of subjects based on validated total DLQI score bands. It showed consistently that omalizumab provides significant and clinically relevant improvements in many aspects of HRQoL that are important to patients with CSU. These results contribute to a better understanding of the impact of CSU and its treatment on patients and can support clinical decision-making in routine medical practice., (© 2017 The Authors. Journal of the European Academy of Dermatology and Venereology published by John Wiley & Sons Ltd on behalf of European Academy of Dermatology and Venereology.)

Published

2017

52. Pathogenesis of Hereditary Angioedema: The Role of the Bradykinin-Forming Cascade.

Author

Kaplan AP and Joseph K

Subjects

Angioedemas, Hereditary metabolism, Bradykinin metabolism, Capillary Permeability, Complement Activation immunology, Complement C1 Inhibitor Protein metabolism, Humans, Signal Transduction, Angioedemas, Hereditary etiology

Abstract

Hereditary angioedema (HAE) is an autosomal-dominant disorder owing to mutations in the C1 inhibitor gene. Type I is characterized by a low C1 inhibitor protein level and diminished functional activity, whereas type II has a normal (or elevated) protein level but diminished function. When functional levels drop beyond 40% of normal, attacks of swelling are likely to occur due to overproduction of bradykinin. Angioedema can be peripheral, abdominal, or laryngeal. The typical duration of episodes is 3 days. Therapies include C1 inhibitor replacement for prophylaxis or acute therapy, whereas inhibition of kallikrein or blockade at the bradykinin receptor level can interrupt acute episodes of swelling., (Copyright © 2017 Elsevier Inc. All rights reserved.)

Published

2017

53. 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

54. Why a registry of Chronic Urticaria (CUR) is needed.

Author

Gómez RM, Jares E, Canonica GW, Baiardini I, Passalacqua G, Sánchez Borges M, Kaplan AP, and Baena-Cagnani CE

Abstract

Chronic urticaria (CU) has a major effect on patients' quality of life. While there have been progressive advances regarding its pathogenesis and treatment, much remains to be done. Registries of other chronic non-communicable diseases have shown many benefits, such as additional basic knowledge and management approaches to diabetes mellitus. Standards of care as well as diagnostic approaches can be elaborated and compared from different sites, using validated instruments. Registries in allergic diseases are also becoming well recognized, and the first registry on CU, accessible from SLaai's webpage, includes parameters for identification, evaluation and management. In our vision, informatics strategies have the potential to improve care for chronic illnesses such as CU. The registry represents a valid instrument from which to obtain a sufficient sample size for epidemiological studies and/or clinical research planning, including feasibility and potential enrollment. It can also provide invaluable data for adapting guidelines to local populations, as well as diagnostic approaches and cost-effective interventions in the context of organizational efforts to improve patient care.

Published

2017

55. Reply.

Author

Joseph K, Constantino-Silva RN, Grumach AS, Feldweg A, Wright L, Frank N, Vuzman D, Sharma R, Suffritti C, Cicardi M, Varga L, Farkas H, Bork K, and Kaplan AP

Subjects

Humans, Plasminogen Activator Inhibitor 2

Published

2017

56. Mechanisms of action that contribute to efficacy of omalizumab in chronic spontaneous urticaria.

Author

Kaplan AP, Giménez-Arnau AM, and Saini SS

Subjects

Agranulocytosis drug therapy, Agranulocytosis etiology, Agranulocytosis metabolism, Animals, Antibodies, Monoclonal, Humanized pharmacology, Antibodies, Monoclonal, Humanized therapeutic use, Autoantibodies immunology, Basophils drug effects, Basophils immunology, Basophils metabolism, Basophils pathology, Chronic Disease, Humans, Immunoglobulin E immunology, Immunoglobulin G immunology, Mast Cells immunology, Mast Cells metabolism, Receptors, IgE metabolism, Treatment Outcome, Urticaria metabolism, Urticaria pathology, Anti-Allergic Agents pharmacology, Anti-Allergic Agents therapeutic use, Omalizumab pharmacology, Omalizumab therapeutic use, Urticaria drug therapy, Urticaria etiology

Abstract

The monoclonal anti-immunoglobulin E (IgE) antibody, omalizumab, was the first drug approved for use in patients with chronic idiopathic/spontaneous urticaria (CIU/CSU) who remain symptomatic despite H 1 -antihistamine treatment. Omalizumab binds to free IgE, which lowers free IgE levels and causes FcεRI receptors on basophils and mast cells to be downregulated. It has been shown to improve symptoms of CIU/CSU, but its mechanism of action is not currently understood. Potential mechanisms in CIU/CSU include reducing mast cell releasability, reversing basopenia and improving basophil IgE receptor function, reducing activity of IgG autoantibodies against FcεRI and IgE, reducing activity of IgE autoantibodies against an antigen or autoantigen that has yet to be definitively identified, reducing the activity of intrinsically 'abnormal' IgE, and decreasing in vitro coagulation abnormalities associated with disease activity. However, none of these theories alone or in combination fully account for the pattern of symptom improvement seen with omalizumab therapy, and therefore, no one mechanism is likely to be the definitive mechanism of action. Additional research is needed to further clarify the involvement of omalizumab in relieving symptoms associated with the complex, multifactorial pathogenesis of CIU/CSU., (© 2016 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2017

57. The complement and contact activation systems: partnership in pathogenesis beyond angioedema.

Author

Ghebrehiwet B, Kaplan AP, Joseph K, and Peerschke EI

Subjects

Animals, Humans, Proteolysis, Receptor Cross-Talk, Signal Transduction, Angioedema immunology, Atherosclerosis immunology, Complement C1q metabolism, Factor XIa metabolism, Immunity, Innate, Inflammation immunology, Neoplasms immunology

Abstract

The blood plasma contains four biologically important proteolytic cascades, which probably evolved from the same ancestral gene. This in part may explain why each cascade has very similar "initiating trigger" followed by sequential and cascade-like downstream enzymatic activation pattern. The four cascades are: the complement system, the blood clotting cascade, the fibrinolytic system, and the kallikrein-kinin system. Although much has been written about the interplay between all these enzymatic cascades, the cross-talk between the complement and the kinin generating systems has become particularly relevant as this interaction results in the generation of nascent molecules that have significant impact in various inflammatory diseases including angioedema and cancer. In this review, we will focus on the consequences of the interplay between the two systems by highlighting the role of a novel molecular link called gC1qR. Although this protein was first identified as a receptor for C1q, it is now recognized as a multiligand binding cellular protein, which serves not only as C1q receptor, but also as high affinity (K D  ≤ 0.8 nM) binding site for both high molecular weight kininogen (HK) and factor XII (FXII). At inflammatory sites, where atherogenic factors such as immune complexes and/or pathogens can activate the endothelial cell into a procoagulant and proinflammatory surface, the two pathways are activated to generate vasoactive peptides that contribute in various ways to the inflammatory processes associated with numerous diseases. More importantly, since recent observations strongly suggest an important role for both pathways in cancer, we will focus on how a growing tumor cluster can employ the byproducts derived from the two activation systems to ensure not only its survival and growth, but also its escape into distal sites of colonization., (© 2016 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2016

58. Fibrinolysis and bradykinin formation: From in vitro observations to human disease in "just" 45 years.

Author

Kaplan AP

Subjects

Angioedemas, Hereditary, Complement C1 Inhibitor Protein, Humans, Bradykinin, Fibrinolysis

Published

2016

59. 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

60. Vibratory Urticaria and ADGRE2.

Author

Kaplan AP, Greenberger PA, and Geller M

Subjects

Female, Humans, Male, Mutation, Missense, Receptors, G-Protein-Coupled genetics, Urticaria genetics, Vibration adverse effects

Published

2016

61. Deficiency of plasminogen activator inhibitor 2 in plasma of patients with hereditary angioedema with normal C1 inhibitor levels.

Author

Joseph K, Tholanikunnel BG, Wolf B, Bork K, and Kaplan AP

Subjects

Angioedemas, Hereditary genetics, Bradykinin blood, Bradykinin metabolism, Case-Control Studies, Complement C1 Inhibitor Protein genetics, Enzyme-Linked Immunosorbent Assay, Factor XII genetics, Female, Humans, Kallikreins metabolism, Male, Mutation, Plasminogen Activator Inhibitor 1 blood, Plasminogen Activator Inhibitor 2 blood, Proteolysis, Angioedemas, Hereditary blood, Angioedemas, Hereditary diagnosis, Complement C1 Inhibitor Protein metabolism, Plasminogen Activator Inhibitor 2 deficiency

Abstract

Background: Hereditary angioedema with normal C1 inhibitor levels (HAE-N) is associated with a Factor XII mutation in 30% of subjects; however, the role of this mutation in the pathogenesis of angioedema is unclear., Objective: We sought evidence of abnormalities in the pathways of bradykinin formation and bradykinin degradation in the plasma of patients with HAE-N both with and without the mutation., Methods: Bradykinin was added to plasma, and its rate of degradation was measured by using ELISA. Plasma autoactivation was assessed by using a chromogenic assay of kallikrein formation. Plasminogen activator inhibitors (PAIs) 1 and 2 were also measured by means of ELISA., Results: PAI-1 levels varied from 0.1 to 4.5 ng/mL (mean, 2.4 ng/mL) in 23 control subjects, from 0.0 to 2 ng/mL (mean, 0.54 ng/mL) in patients with HAE-N with a Factor XII mutation (12 samples), and from 0.0 to 3.7 ng/mL (mean, 1.03 ng/mL) in patients with HAE-N without a Factor XII mutation (11 samples). PAI-2 levels varied from 25 to 87 ng/mL (mean, 53.8 ng/mL) in control subjects and were 0 to 25 ng/mL (mean, 4.3 ng/mL) in patients with HAE-N with or without the Factor XII mutation. Autoactivation at a 1:2 dilution was abnormally high in 8 of 17 patients with HAE-N (4 in each subcategory) and could be corrected by supplemental C1 inhibitor in 4 of them. Bradykinin degradation was markedly abnormal in 1 of 23 patients with HAE-N and normal in the remaining 22 patients., Conclusions: Bradykinin degradation was normal in all but 1 of 23 patients with HAE-N studied. By contrast, there was a marked abnormality in PAI-2 levels in patients with HAE-N that is not seen in patients with C1 inhibitor deficiency. PAI-1 levels varied considerably, but a statistically significant difference was not seen. A link between excessive fibrinolysis and bradykinin generation that is estrogen dependent is suggested., (Copyright © 2015 American Academy of Allergy, Asthma & Immunology. Published by Elsevier Inc. All rights reserved.)

Published

2016

62. Similar Efficacy with Omalizumab in Chronic Idiopathic/Spontaneous Urticaria Despite Different Background Therapy.

Author

Casale TB, Bernstein JA, Maurer M, Saini SS, Trzaskoma B, Chen H, Grattan CE, Gimenéz-Arnau A, Kaplan AP, and Rosén K

Subjects

Adult, Analysis of Variance, Chronic Disease, Drug Dosage Calculations, Drug Therapy, Combination, Female, Follow-Up Studies, Histamine H1 Antagonists adverse effects, Histamine H2 Antagonists adverse effects, Humans, Male, Middle Aged, Omalizumab adverse effects, Recurrence, Treatment Outcome, Urticaria immunology, Histamine H1 Antagonists administration & dosage, Histamine H2 Antagonists administration & dosage, Immunotherapy methods, Omalizumab administration & dosage, Urticaria therapy

Abstract

Background: Data from the 3 omalizumab pivotal trials in patients with chronic idiopathic urticaria/chronic spontaneous urticaria (CIU/CSU) represent the largest database of patients reported to date with refractory disease (omalizumab, n = 733; placebo, n = 242)., Objective: The objective of this study was to compare results from ASTERIA I and II, which included only approved doses of H1-antihistamine as background therapy based on regulatory authority requirements, to those from GLACIAL, which permitted higher doses of H1-antihistamines as well as other types of background therapy, in a post hoc analysis., Methods: Efficacy data from the placebo, omalizumab 150-mg, and omalizumab 300-mg treatment arms of ASTERIA I and II were pooled and analyzed (n = 162 and n = 160, respectively). The 300-mg treatment arm analyses were compared with the analysis of data from GLACIAL (n = 252) using analysis of covariance models. The key efficacy endpoint was change from baseline to week 12 in mean weekly itch severity score (ISS); other endpoints were also evaluated. Safety data were pooled from all 3 studies., Results: Mean ISS was significantly reduced from baseline at week 12 in the pooled ASTERIA I and II omalizumab 150- and 300-mg treatment arms and in the GLACIAL omalizumab 300-mg arm. The weekly ISS reduction magnitude at week 12 was similar between the omalizumab 300-mg groups in the ASTERIA I and II pooled and GLACIAL studies. Similar treatment effect sizes were observed across multiple endpoints. Omalizumab was well tolerated and the adverse-event profile was similar regardless of background therapy for CIU/CSU. The overall safety profile was generally consistent with omalizumab therapy in allergic asthma., Conclusion: Omalizumab 300 mg was safe and effective in reducing CIU/CSU symptoms regardless of background therapy., (Copyright © 2015 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2015

63. How omalizumab came to be studied as a therapy for chronic spontaneous/idiopathic urticaria.

Author

Kaplan AP, Joseph K, and Saini SS

Subjects

Humans, Anti-Allergic Agents therapeutic use, Anti-Asthmatic Agents therapeutic use, Immunoglobulin E immunology, Omalizumab therapeutic use

Published

2015

64. In vitro comparison of bradykinin degradation by aliskiren, a renin inhibitor, and an inhibitor of angiotensin-converting enzyme.

Author

Joseph K, Tholanikunnel TE, and Kaplan AP

Subjects

3-Mercaptopropionic Acid analogs & derivatives, 3-Mercaptopropionic Acid pharmacology, Bradykinin blood, Endothelial Cells drug effects, Endothelial Cells metabolism, Humans, Pulmonary Artery cytology, Amides pharmacology, Angiotensin-Converting Enzyme Inhibitors pharmacology, Bradykinin metabolism, Fumarates pharmacology, Peptidyl-Dipeptidase A metabolism, Renin antagonists & inhibitors

Abstract

Introduction: Angiotensin-converting enzyme (ACE) inhibitors cause angioedema due to diminished degradation of bradykinin. Angiotensin receptor blockers may occasionally cause angioedema but the mechanism is unknown, and are generally considered safe, even in those who have reacted to ACE inhibitors. We determined whether aliskiren, a renin inhibitor, has an effect on the rate of bradykinin degradation., Methods: The ability of renin to metabolize bradykinin was studied and the rate of bradykinin degradation compared in the presence or absence of aliskiren. Enalapril, a known ACE inhibitor that causes angioedema served as positive control., Results: Renin was unable to digest bradykinin, indicating that a renin inhibitor is unlikely to affect the rate of bradykinin degradation. In a plasma system, aliskiren had no effect on the rate of bradykinin degradation while enalapril inhibited it appreciably. An inhibitory effect of aliskiren on the rate of bradykinin degradation by human pulmonary endothelial cells was observed, estimated to be about 5% of that of enalapril., Conclusion: Aliskiren has no effect upon the rate of bradykinin degradation in plasma and a minimal effect employing vascular endothelial cells. The latter suggests inhibition of a non-renin enzyme that is a minor contributor to bradykinin degradation., (© The Author(s) 2013.)

Published

2015

65. Neurotropin promotes NGF signaling through interaction of GM1 ganglioside with Trk neurotrophin receptor in PC12 cells.

Author

Fukuda Y, Fukui T, Hikichi C, Ishikawa T, Murate K, Adachi T, Imai H, Fukuhara K, Ueda A, Kaplan AP, and Mutoh T

Subjects

Animals, Carbazoles pharmacology, Cell Differentiation drug effects, Dimerization, Dose-Response Relationship, Drug, Indole Alkaloids pharmacology, Neurites drug effects, PC12 Cells, Rats, Time Factors, Analgesics pharmacology, G(M1) Ganglioside metabolism, Nerve Growth Factor metabolism, Polysaccharides pharmacology, Receptor Protein-Tyrosine Kinases metabolism, Signal Transduction drug effects

Abstract

Activation of the high-affinity nerve growth factor (NGF) receptor Trk occurs through multiple processes consisted of translocation and clustering within the plasma membrane lipid rafts, dimerization and autophosphorylation. Here we found that a nonprotein extract of inflamed rabbit skin inoculated with vaccinia virus (Neurotropin(®)) enhanced efficiency of NGF signaling. In rat pheochromocytoma PC12 cells overexpressing Trk (PCtrk cells), Neurotropin augmented insufficient neurite outgrowth observed at suboptimal concentration of NGF (2ng/mL) in a manner depending on Trk kinase activity. Cellular exposure to Neurotropin resulted in an accumulation of Trk-GM1 complexes without affecting dimerization or phosphorylation states of Trk. Following NGF stimulation, Neurotropin significantly facilitated the time course of NGF-induced Trk autophosphorylation. These observations provide a unique mechanism controlling efficiency of NGF signaling, and raise the therapeutic potential of Neurotropin for various neurological conditions associated with neurotrophin dysfunction., (Copyright © 2014 Elsevier B.V. All rights reserved.)

Published

2015

66. A novel assay to diagnose hereditary angioedema utilizing inhibition of bradykinin-forming enzymes.

Author

Joseph K, Bains S, Tholanikunnel BG, Bygum A, Aabom A, Koch C, Farkas H, Varga L, Ghebrehiwet B, and Kaplan AP

Subjects

Angioedemas, Hereditary enzymology, Case-Control Studies, Complement C1 Inhibitor Protein metabolism, Enzyme-Linked Immunosorbent Assay, Humans, Reproducibility of Results, Sensitivity and Specificity, Angioedemas, Hereditary diagnosis, Bradykinin biosynthesis, Factor XIIa, Plasma Kallikrein

Abstract

Background: Hereditary angioedema types I and II are caused by a functional deficiency of C1 inhibitor (C1-INH), leading to overproduction of bradykinin. The current functional diagnostic assays employ inhibition of activated C1s; however, an alternative, more physiologic method is desirable., Methods: ELISAs were developed using biotinylated activated factor XII (factor XIIa) or biotinylated kallikrein bound to avidin-coated plates. Incubation with plasma was followed by detection of bound C1-INH., Results: After standard curves were developed for quantification of C1-INH, serial dilutions of normal plasma were employed to validate the ability to detect known concentration of C1-INH in the plasma as a percent of normal. Hereditary angioedema (HAE) types I and II were then tested. The level of functional C1-INH in all HAE types I and II plasma tested was less than 40% of our normal control. This was evident regardless of whether we measured factor XIIa-C1-INH or kallikrein-C1-INH complexes, and the two assays were in close agreement. By contrast, testing the same samples utilizing the commercial method (complex ELISA, Quidel Corp.) revealed the levels of C1-INH between 0 and 57% of normal (mean, 38%), and 42 samples were considered equivocal (four controls and 38 patients)., Conclusions: Diagnosis of HAE types I and II can be ascertained by inhibition of enzymes of the bradykinin-forming cascade, namely factor XIIa and kallikrein. Either method yields functional C1-INH levels in patients with HAE (types I and II) that are clearly abnormal with less variance or uncertainty than the commercial method., (© 2014 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2015

67. The thrombogenicity of C1 esterase inhibitor (human): review of the evidence.

Author

Crowther M, Bauer KA, and Kaplan AP

Subjects

Angioedemas, Hereditary blood, Angioedemas, Hereditary complications, Angioedemas, Hereditary drug therapy, Animals, Blood Coagulation drug effects, Complement C1 Inhibitor Protein administration & dosage, Complement C1 Inhibitor Protein therapeutic use, Disease Models, Animal, Humans, Incidence, Risk Factors, Thrombosis epidemiology, Complement C1 Inhibitor Protein adverse effects, Thrombosis chemically induced

Abstract

Thromboembolic events associated with human plasma-derived C1 esterase inhibitor (C1-INH) use in patients with hereditary angioedema (HAE) have been reported in the U.S. Food and Drug Administration (FDA) Adverse Event Reporting System database. The purpose of this article is to review and assess the strength of available evidence regarding the thrombogenicity of human plasma-derived C1-INH. A PubMed search was conducted of English language articles from January 1990 to December 2013 reporting the thrombogenicity of C1-INH. Original research articles were selected if the following criteria were met: (1) C1-INH was the focus of the study and (2) the authors addressed the pro- or antithrombotic potential of C1-INH. Additional articles on the clinical use of C1-INH in disease states other than HAE were obtained using reference lists of selected articles. Pivotal studies and prescribing information for C1-INH products were also reviewed. Limited animal and clinical data suggest that C1-INH, particularly at high doses of up to 500 U/kg (compared with the U.S. FDA-approved 20-U/kg dose), may be prothrombotic. In contrast, C1-INH has been used in some patients with myocardial infarction, ischemic stroke, sepsis, and capillary leak syndrome at off-label supratherapeutic doses (up to 100 U/kg) without evidence of a thrombogenic effect. Based on our review, thromboembolic events reported with C1-INH use are rare and patients with HAE who experienced such events often have underlying thromboembolic risk factors.

Published

2014

68. Biologic agents and the therapy of chronic spontaneous urticaria.

Author

Kaplan AP and Popov TA

Subjects

Anti-Allergic Agents administration & dosage, Anti-Allergic Agents therapeutic use, Antibodies, Anti-Idiotypic administration & dosage, Antibodies, Anti-Idiotypic therapeutic use, Antibodies, Monoclonal, Humanized administration & dosage, Antibodies, Monoclonal, Humanized therapeutic use, Clinical Trials as Topic, Humans, Omalizumab, Anti-Allergic Agents pharmacology, Antibodies, Anti-Idiotypic pharmacology, Antibodies, Monoclonal, Humanized pharmacology, Urticaria drug therapy

Abstract

Purpose of Review: Chronic spontaneous urticaria (CSU) has been traditionally managed with antihistamines. Over the years, studies using different formulations and dosing regimens have delineated the limits of their effectiveness, thus emphasizing the need for alternative therapeutic approaches. Data keep accumulating that the monoclonal anti-immunoglobulin E antibody omalizumab, until recently reserved for the treatment of severe atopic asthma, may have a beneficial therapeutic and safety profile for CSU cases resistant to the effect of antihistamines., Recent Findings: Since the beginning of 2013, a host of studies have been published paving the way for licensing of omalizumab for the treatment of CSU. Dose-finding studies have indicated 300 mg monthly as a possible optimal treatment regimen. Efficacy proving randomized controlled trials were further supported by open-label studies confirming its effectiveness in real life. One report has been published so far presenting positive data about the use of another biologic agent, rituximab, depleting the blood stream of B cells, in patients with CSU., Summary: New convincing evidence in support of the efficacy and safety of omalizumab in the treatment of CSU has accumulated over the past year, providing another tool for coping with the antihistamine-resistant cases.

Published

2014

69. Therapy of chronic urticaria: a simple, modern approach.

Author

Kaplan AP

Subjects

Anti-Allergic Agents adverse effects, Antibodies, Anti-Idiotypic adverse effects, Antibodies, Monoclonal, Humanized adverse effects, Chronic Disease, Cyclosporine adverse effects, Cyclosporine therapeutic use, Histamine Antagonists therapeutic use, Humans, Immunosuppressive Agents therapeutic use, Omalizumab, Urticaria pathology, Anti-Allergic Agents therapeutic use, Antibodies, Anti-Idiotypic therapeutic use, Antibodies, Monoclonal, Humanized therapeutic use, Urticaria drug therapy

Abstract

Objective: To examine the available treatment choices for chronic spontaneous urticaria (CSU) and discuss a new paradigm for treating such patients., Data Sources: The literature regarding treatment is reviewed, including considerations of published guidelines. Attention is focused on the most recent evidence indicating particular efficacy of omalizumab., Results: Omalizumab has been found to have considerable efficacy in phase 2 and phase 3 trials in which more than 900 patients have been studied. A response rate of 65% is seen in patients resistant to antihistamines as well as to histamine2 blockers and leukotriene antagonists, and 40% of patients are completely free of hives as long as therapy is continued. In addition, serious adverse events have not been seen. Only cyclosporine can match this response rate (excluding steroids), but the adverse effect profile (blood pressure and renal function) is substantial by comparison. Double-blind, placebo-controlled studies of other agents often listed as alternatives are lacking (ie, whether their success rate exceeds the 25%-30% placebo response is uncertain). The mechanism by which omalizumab works in CSU is not clear because the response rate is unrelated to the autoimmune profile and can occur rapidly (ie, within a few days)., Conclusion: Omalizumab has exceptional efficacy for antihistamine-resistant CSU with an excellent adverse effect profile., (Copyright © 2014 American College of Allergy, Asthma & Immunology. Published by Elsevier Inc. All rights reserved.)

Published

2014

70. Classification, diagnosis, and approach to treatment for angioedema: consensus report from the Hereditary Angioedema International Working Group.

Author

Cicardi M, Aberer W, Banerji A, Bas M, Bernstein JA, Bork K, Caballero T, Farkas H, Grumach A, Kaplan AP, Riedl MA, Triggiani M, Zanichelli A, and Zuraw B

Subjects

Angioedema etiology, Humans, Angioedema diagnosis, Angioedema drug therapy

Abstract

Angioedema is defined as localized and self-limiting edema of the subcutaneous and submucosal tissue, due to a temporary increase in vascular permeability caused by the release of vasoactive mediator(s). When angioedema recurs without significant wheals, the patient should be diagnosed to have angioedema as a distinct disease. In the absence of accepted classification, different types of angioedema are not uniquely identified. For this reason, the European Academy of Allergy and Clinical Immunology gave its patronage to a consensus conference aimed at classifying angioedema. Four types of acquired and three types of hereditary angioedema were identified as separate forms from the analysis of the literature and were presented in detail at the meeting. Here, we summarize the analysis of the data and the resulting classification of angioedema., (© 2014 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2014

71. Bradykinin in health and disease: proceedings of the Bradykinin Symposium 2012, Berlin 23-24 August 2012.

Author

Magerl M, Bader M, Gompel A, Joseph K, Kaplan AP, Kojda G, Renné T, Wirth M, Maurer M, and Church MK

Subjects

Angioedemas, Hereditary drug therapy, Angiotensin-Converting Enzyme Inhibitors, Animals, Bradykinin metabolism, Disease, Endothelium physiology, Estrogens physiology, Factor XII physiology, Health, Humans, Nitric Oxide physiology, Receptors, Bradykinin physiology, Bradykinin physiology

Published

2014

72. The maddening itch: an approach to chronic urticaria.

Author

Viegas LP, Ferreira MB, and Kaplan AP

Subjects

Antibodies, Anti-Idiotypic therapeutic use, Antibodies, Monoclonal, Humanized therapeutic use, Chronic Disease, Cyclosporine therapeutic use, Humans, Immunosuppressive Agents therapeutic use, Omalizumab, Pruritus immunology, Urticaria immunology, Histamine Antagonists therapeutic use, Pruritus diagnosis, Pruritus drug therapy, Urticaria diagnosis, Urticaria drug therapy

Abstract

Chronic spontaneous urticaria (CSU) is defined as the presence of urticaria with daily or almost daily symptoms for 6 weeks or more. CSU affects 0.1%-0.8% of the population. Its pathogenesis involves autoimmunity, abnormalities in signal transduction, and the action of histamine on H1 receptors. Investigation of CSU should be guided by a thorough history and physical examination. A concise laboratory evaluation, including the CU index, is recommended. This index can provide useful data on severity and response to therapy. Initial treatment should involve increasing doses of nonsedating antihistamines until the intended effect is achieved. Only when a patient is unresponsive to high-dose nonsedating antihistamines (or sedating antihistamines) can we consider CSU refractory and consider immunomodulatory therapy. The most promising drugs are cyclosporine and, more recently, omalizumab.

Published

2014

73. Bradykinin-mediated diseases.

Author

Kaplan AP

Subjects

Angioedema drug therapy, Angioedema immunology, Angioedemas, Hereditary drug therapy, Angioedemas, Hereditary etiology, Angioedemas, Hereditary immunology, Angiotensin-Converting Enzyme Inhibitors adverse effects, Angiotensin-Converting Enzyme Inhibitors therapeutic use, Anti-Inflammatory Agents, Non-Steroidal therapeutic use, Antifibrinolytic Agents therapeutic use, Bradykinin analogs & derivatives, Bradykinin blood, Complement C1 antagonists & inhibitors, Complement C1 genetics, Complement C1 metabolism, Factor XII metabolism, Humans, Kallikreins antagonists & inhibitors, Kallikreins metabolism, Angioedema etiology, Bradykinin metabolism

Abstract

Diseases which have been demonstrated to be caused by increased plasma levels of bradykinin all have angioedema as the common major clinical manifestation. Angioedema due to therapy with angiotensin-converting enzyme (ACE) inhibitors is caused by suppressed bradykinin degradation so that it accumulates. This occurs because ACE metabolizes bradykinin by removal of Phe-Arg from the C-terminus, which inactivates it. By contrast, angioedema due to C1 inhibitor deficiency (either hereditary types I and II, or acquired) is caused by bradykinin overproduction. C1 inhibitor inhibits factor XIIa, kallikrein and activity associated with the prekallikrein-HK (high-molecular-weight kininogen) complex. In its absence, uncontrolled activation of the plasma bradykinin cascade is seen once there has been an initiating stimulus. C4 levels are low in all types of C1 inhibitor deficiency due to the instability of C1 (C1r, in particular) such that some activated C1 always circulates and depletes C4. In the hereditary disorder, formation of factor XIIf (factor XII fragment) during attacks of swelling causes C4 levels to drop toward zero, and C2 levels decline. A kinin-like molecule, once thought to be a cleavage product derived from C2 that contributes to the increased vascular permeability seen in hereditary angioedema (HAE), is now thought to be an artifact, i.e. no such molecule is demonstrable. The acquired C1 inhibitor deficiency is associated with clonal disorders of B cell hyperreactivity, including lymphoma and monoclonal gammopathy. Most cases have an IgG autoantibody to C1 inhibitor which inactivates it so that the presentation is strikingly similar to type I HAE. New therapies for types I and II HAE include C1 inhibitor replacement therapy, ecallantide, a kallikrein antagonist, and icatibant, a B2 receptor antagonist. A newly described type III HAE has normal C1 inhibitor, although it is thought to be mediated by bradykinin, as is an antihistamine-resistant subpopulation of patients with 'idiopathic' angioedema. The mechanism(s) for the formation of bradykinin in these disorders is unknown., (© 2014 S. Karger AG, Basel.)

Published

2014

74. Pathogenic mechanisms of bradykinin mediated diseases: dysregulation of an innate inflammatory pathway.

Author

Kaplan AP and Joseph K

Subjects

Angioedemas, Hereditary etiology, Animals, Bradykinin blood, Bradykinin physiology, Complement C1 Inhibitor Protein physiology, Endothelium, Vascular immunology, Endothelium, Vascular metabolism, Endothelium, Vascular pathology, Factor XII metabolism, Factor XII physiology, Humans, Inflammation blood, Inflammation immunology, Inflammation pathology, Inflammation Mediators blood, Kininogen, High-Molecular-Weight physiology, Prekallikrein physiology, Angioedemas, Hereditary immunology, Angioedemas, Hereditary pathology, Bradykinin metabolism, Immunity, Innate, Inflammation Mediators physiology, Signal Transduction immunology

Abstract

Binding of negatively charged macromolecules to factor XII induces a conformational change such that it becomes a substrate for trace amounts of activated factor present in plasma (less than 0.01%). As activated factor XII (factor XIIa or factor XIIf) forms, it converts prekallikrein (PK) to kallikrein and kallikrein cleaves high molecular weight kininogen (HK) to release bradykinin. A far more rapid activation of the remaining unactivated factor XII occurs by enzymatic cleavage by kallikrein (kallikrein-feedback) and sequential cleavage yields two forms of activated factor XII; namely, factor XIIa followed by factor XII fragment (factor XIIf). PK circulates bound to HK and binding induces a conformational change in PK so that it acquires enzymatic activity and can stoichiometrically cleave HK to produce bradykinin. This reaction is prevented from occurring in plasma by the presence of C1 inhibitor (C1 INH). The same active site leads to autoactivation of the PK-HK complex to generate kallikrein if a phosphate containing buffer is used. Theoretically, formation of kallikrein by this factor XII-independent route can activate surface-bound factor XII to generate factor XIIa resulting in a marked increase in the rate of bradykinin formation as stoichiometric reactions are replaced by Michaelis-Menton, enzyme-substrate, kinetics. Zinc-dependent binding of the constituents of the bradykinin-forming cascade to the surface of endothelial cells is mediated by gC1qR and bimolecular complexes of gC1qR-cytokeratin 1 and cytokeratin 1-u-PAR (urokinase plasminogen activator receptor). Factor XII and HK compete for binding to free gC1qR (present in excess) while cytokeratin 1-u-PAR preferentially binds factor XII and gC1qR-cytokeratin 1 preferentially binds HK. Autoactivation of factor XII can be initiated as a result of binding to gC1qR but is prevented by C1 INH. Yet stoichiometric activation of PK-HK to yield kallikrein in the absence of factor XII can be initiated by heat shock protein 90 (HSP-90) which forms a zinc-dependent trimolecular complex by binding to HK. Thus, endothelial cell-dependent activation can be initiated by activation of factor XII or by activation of PK-HK. Hereditary angioedema (HAE), types I and II, are due to autosomal dominant mutations of the C1 INH gene. In type I disease, the level of C1 INH protein and function is proportionately low, while type II disease has a normal protein level but diminished function. There is trans-inhibition of the one normal gene so that functional levels are 30% or less and severe angioedema affecting peripheral structures, the gastrointestinal tract, and the larynx results. Prolonged incubation of plasma of HAE patients (but not normal controls) leads to bradykinin formation and conversion of PK to kallikrein which is reversed by reconstitution with C1 INH. The disorder can be treated by C1 INH replacement, inhibition of plasma kallikrein, or blockade at the bradykinin B-2 receptor. A recently described HAE with normal C1 INH (based on inhibition of activated C1s) presents similarly; the defect is not yet clear, however one-third of patients have a mutant factor XII gene. We have shown that this HAE has a defect in bradykinin overproduction whether the factor XII mutation is present or not, that patients' C1 INH is capable of inhibiting factor XIIa and kallikrein (and not just activated C1) but the functional level is approximately 40-60% of normal, and that α2 macroglobulin protein levels are normal. In vitro abnormalities can be suppressed by raising C1 INH to twice normal levels. Finally, aggregated proteins have been shown to activate the bradykinin-forming pathway by catalyzing factor XII autoactivation. Those include the amyloid β protein of Alzheimer's disease and cryoglobulins. This may represent a new avenue for kinin-dependent research in human disease. In allergy (anaphylaxis; perhaps other mast cell-dependent reactions), the oversulfated proteoglycan of mast cells, liberated along with histamine, also catalyze factor XII autoactivation., (© 2014 Elsevier Inc. All rights reserved.)

Published

2014

75. The bradykinin-forming cascade: a historical perspective.

Author

Kaplan AP

Subjects

Bradykinin chemistry, Endothelial Cells metabolism, Factor XII chemistry, Factor XII metabolism, HSP90 Heat-Shock Proteins metabolism, Humans, Kininogen, High-Molecular-Weight chemistry, Kininogen, High-Molecular-Weight metabolism, Prekallikrein chemistry, Prekallikrein metabolism, Protein Binding, Protein Structure, Tertiary, Bradykinin metabolism

Abstract

The formation of bradykinin in plasma requires interaction of three proteins, namely coagulation factor XII (Hageman factor), prekallikrein and high-molecular-weight kininogen (HK). Prekallikrein and HK circulate as a bimolecular complex. Initiation of the cascade upon binding to negatively charged surfaces (or macromolecules) is dependent on factor XII autoactivation, conversion of prekallikrein to kallikrein, and a feedback activation of factor XII by kallikrein. The latter reaction is extremely rapid relative to factor XII autoactivation. The kallikrein then digests HK to liberate bradykinin. The natural surface appears to be vascular endothelial cells which express binding proteins for factor XII and HK, and activation can proceed along the cell surface. Recent findings demonstrate that prekallikrein has enzymatic activity separate from that of kallikrein such that it can stoichiometrically bind and cleave HK to liberate bradykinin. It is normally prevented from doing so by the plasma C1 inhibitor. Release of heat shock protein 90 (HSP-90) from endothelial cells can convert prekallikrein to kallikrein (stoichiometrically) within the prekallikrein-HK complex, even in the absence of factor XII, and the prekallikrein-HK complex can autoactivate to generate kallikrein if phosphate is the buffering ion. The effects of phosphate ion and HSP-90 are additive. Thus, an active site appears to be induced in prekallikrein by binding to HK and any of the aforementioned reactions can generate kallikrein prior to factor XII activation by autoactivation of the HK-PK complex. This brief review highlights the major discoveries made over the past 50 years which have led to our current concepts regarding the constituents and mechanisms of activation of the plasma bradykinin-forming cascade., (© 2014 S. Karger AG, Basel.)

Published

2014

76. Factor XII-independent activation of the bradykinin-forming cascade: Implications for the pathogenesis of hereditary angioedema types I and II.

Author

Joseph K, Tholanikunnel BG, Bygum A, Ghebrehiwet B, and Kaplan AP

Subjects

Complement C1 Inactivator Proteins metabolism, Complement C1 Inhibitor Protein, Female, HSP90 Heat-Shock Proteins metabolism, Humans, Kallikreins metabolism, Male, Angioedemas, Hereditary physiopathology, Bradykinin metabolism, Factor XII metabolism, Hereditary Angioedema Types I and II physiopathology, Kininogen, High-Molecular-Weight metabolism, Prekallikrein metabolism

Abstract

Background: We have previously reported that prekallikrein expresses an active site when it is bound to high-molecular-weight kininogen (HK) and can digest HK to produce bradykinin. The reaction is stoichiometric and inhibited by C1 inhibitor (C1-INH) or corn trypsin inhibitor. Addition of heat shock protein 90 leads to conversion of prekallikrein to kallikrein in a zinc-dependent reaction., Objective: Our goal was to determine whether these reactions are demonstrable in plasma and distinguish them from activation through factor XII., Methods: Plasma was incubated in polystyrene plates and assayed for kallikrein formation. C1-INH was removed from factor XII-deficient plasma by means of immunoadsorption., Results: We demonstrate that prekallikrein-HK will activate to kallikrein in phosphate-containing buffers and that the rate is further accelerated on addition of heat shock protein 90. Prolonged incubation of plasma deficient in both factor XII and C1-INH led to conversion of prekallikrein to kallikrein and cleavage of HK, as was seen in plasma from patients with hereditary angioedema but not plasma from healthy subjects., Conclusions: These results indicate that C1-INH stabilizes the prekallikrein-HK complex to prevent HK cleavage either by prekallikrein or by prekallikrein-HK autoactivation to generate kallikrein. In patients with hereditary angioedema, kallikrein and bradykinin formation can occur without invoking factor XII activation, although the kallikrein formed can rapidly activate factor XII if it is surface bound., (Copyright © 2013 American Academy of Allergy, Asthma & Immunology. Published by Mosby, Inc. All rights reserved.)

Published

2013

77. Chronic idiopathic urticaria (CIU) is no longer idiopathic: time for an update.

Author

Maurer M, Bindslev-Jensen C, Gimenez-Arnau A, Godse K, Grattan CE, Hide M, Kaplan AP, Makris M, Simons FE, Zhao Z, Zuberbier T, and Church MK

Subjects

Chronic Disease, Humans, Terminology as Topic, Urticaria classification

Published

2013

78. Treatment of chronic spontaneous urticaria.

Author

Kaplan AP

Abstract

Chronic spontaneous urticaria is defined as persistent symptoms of urticaria for 6 weeks or more. It is associated with autoimmunity in approximately 45 percent of patients. Therapy is often difficult however the initial approach should employ high-dose non-sedating antihistamines; 4-6 tablets/day may be necessary. It has been shown that the response to 4 tablets/day exceeds 3, and exceeds 2, which exceeds 1. However the dose that corresponds to the maximal dose of first generation antihistamines (hydroxyzine, diphenhydramine) used previously, is 6/day. Yet over half the patients are refractory to antihistamines and other agents should be tried next. Whereas current guidelines (published) often add leukotriene antagonists and/or H(2) receptor antogonists next, these are of little utility. Likewise drugs effective for urticarial vasculitis (colchicine, dapsone, sulfasalazine, hydroxychloroquine) are effective in a small percentage of patients and no study suggests that the response rate of any of them exceeds the 30% placebo responses seen in most double-blind, placebo controlled studies. The drugs that are effective for antihistamine-resistant chronic spontaneous urticaria are corticosteroids, cyclosporine, and Omalizumab. Use of steroids is limited by toxicity. If used at all, a dose of no more than 10 mg/day should be employed with a weekly reduction of 1 mg. The response rates to cyclosporine and Omalizumab are each close to 75%. Cyclosporine can be used effectively if care is taken to monitor blood pressure, urine protein, blood urea nitrogen, and creatinine, every 6 weeks. Omalizumab has the best profile in terms of efficacy/toxicity and, once approved by federal agencies for use in chronic spontaneous urticaria, a dramatic change in the treatment paradigm, whether associated with autoimmunity or not, is predicted. A phase 3 trial is currently in place. Refractoriness to both Omalizumab and cyclosporine is expected to be less than 5 percent of patients. Other agents, can then be tried.

Published

2012

79. Diagnosis and treatment of urticaria and angioedema: a worldwide perspective.

Author

Sánchez-Borges M, Asero R, Ansotegui IJ, Baiardini I, Bernstein JA, Canonica GW, Gower R, Kahn DA, Kaplan AP, Katelaris C, Maurer M, Park HS, Potter P, Saini S, Tassinari P, Tedeschi A, Ye YM, and Zuberbier T

Abstract

: Urticaria and angioedema are common clinical conditions representing a major concern for physicians and patients alike. The World Allergy Organization (WAO), recognizing the importance of these diseases, has contributed to previous guidelines for the diagnosis and management of urticaria. The Scientific and Clinical Issues Council of WAO proposed the development of this global Position Paper to further enhance the clinical management of these disorders through the participation of renowned experts from all WAO regions of the world. Sections on definition and classification, prevalence, etiology and pathogenesis, diagnosis, treatment, and prognosis are based on the best scientific evidence presently available. Additional sections devoted to urticaria and angioedema in children and pregnant women, quality of life and patient-reported outcomes, and physical urticarias have been incorporated into this document. It is expected that this article will supplement recent international guidelines with the contribution of an expert panel designated by the WAO, increasing awareness of the importance of urticaria and angioedema in medical practice and will become a useful source of information for optimum patient management worldwide.

Published

2012

80. Biologic agents in the treatment of urticaria.

Author

Kaplan AP

Subjects

Anti-Allergic Agents therapeutic use, Antibodies, Anti-Idiotypic therapeutic use, Antibodies, Monoclonal, Humanized therapeutic use, Clinical Trials as Topic, Cyclosporine therapeutic use, Humans, Omalizumab, Urticaria immunology, Urticaria drug therapy

Abstract

Numerous controlled studies as well as case reports have demonstrated that Omalizumab can be employed successfully in approximately 75 % of patients with chronic spontaneous urticaria, leading to a dramatic decrement in symptoms with very few side effects. No other drug currently available is comparable, and the success rate in patients resistant to antihistamines is no different. In the U.S., Phase I and Phase II trials are complete and we await the results of a Phase III multicenter study, with a view to eventual submission to the Food and Drug Administration in the U.S. and to comparable agencies abroad seeking approval for this indication. Omalizumab is currently marketed for the treatment of severe allergic asthma. Case reports suggest efficacy in difficult cases of physical urticaria, but no controlled trails have been done. Other agents require further evaluation for possible efficacy in the treatment of chronic spontaneous urticaria, including antibody to CD20, a B-lymphocyte cell surface marker, anti-TNFα, and anti-Interleukin 1. Thus far, targeting TNFα has been disappointing for this indication, while targeting Interleukin I has dramatically ameliorated autoinflammatory disorders with urticaria or urticaria-vasculitic-like lesions such as cold-induced autoinflammatory syndrome, Muckle-Wells syndrome, and Schnitzler syndrome.

Published

2012

81. Structure-function studies using deletion mutants identify domains of gC1qR/p33 as potential therapeutic targets for vascular permeability and inflammation.

Author

Ghebrehiwet B, Jesty J, Xu S, Vinayagasundaram R, Vinayagasundaram U, Ji Y, Valentino A, Hosszu KK, Mathew S, Joseph K, Kaplan AP, and Peerschke EI

Abstract

The endothelial cell receptor complex for kininogen (HK) comprises gC1qR, cytokeratin 1, and urokinase-type plasminogen activator receptor and is essential for activation of the kinin system that leads to bradykinin (BK) generation. Of these, gC1qR/p33 constitutes a high affinity site for HK - the BK precursor - and is therefore critical for the assembly of the kinin-generating cascade. Previous studies have identified a putative HK site within the C-terminal domain (residues 204-218) of gC1qR recognized by mAb 74.5.2. In these studies, we used information from the crystal structure of gC1qR, to engineer several deletion (Δ) mutants and test their ability to bind and/or support BK generation. While deletion of residues 204-218 (gC1qRΔ204-218), showed significantly reduced binding to HK, BK generation was not affected when tested by a sensitive bradykinin immunoassay. In fact, all of the gC1qR deletion mutants supported BK generation with the exception of gC1qRΔ154-162 and a point mutation in which Trp 233 was substituted with Gly. Binding studies also identified the existence of two additional sites at residues 144-162 and 190-202. Moreover, binding of HK to a synthetic peptide 190-202 was inhibited by mAbs 48 and 83, but not by mAb 74.5.2. Since a single residue separates domains 190-202 and 204-218, they may be part of a highly stable HK binding pocket and therefore a potential target for drug design to prevent vascular permeability and inflammation.

Published

2011

82. History of the World Allergy Organization: 1989 to 2006, the XVIII World Allergy Congress, Journal Development, Reorganization, and New Programs.

Author

Kaplan AP

Published

2011

83. Safety and tolerability of the direct renin inhibitor aliskiren in combination with angiotensin receptor blockers and thiazide diuretics: a pooled analysis of clinical experience of 12,942 patients.

Author

White WB, Bresalier R, Kaplan AP, Palmer BF, Riddell RH, Lesogor A, Chang W, and Keefe DL

Subjects

Adult, Adverse Drug Reaction Reporting Systems, Aged, Antihypertensive Agents administration & dosage, Antihypertensive Agents adverse effects, Antihypertensive Agents pharmacokinetics, Biological Availability, Drug Interactions, Drug Monitoring, Drug Therapy, Combination, Female, Humans, Hypertension metabolism, Hypertension physiopathology, Male, Middle Aged, Randomized Controlled Trials as Topic, Renin metabolism, Treatment Outcome, Amides administration & dosage, Amides adverse effects, Amides pharmacokinetics, Angiotensin Receptor Antagonists administration & dosage, Angiotensin Receptor Antagonists adverse effects, Angiotensin Receptor Antagonists pharmacokinetics, Blood Pressure drug effects, Fumarates administration & dosage, Fumarates adverse effects, Fumarates pharmacokinetics, Hypertension drug therapy, Sodium Chloride Symporter Inhibitors administration & dosage, Sodium Chloride Symporter Inhibitors adverse effects, Sodium Chloride Symporter Inhibitors pharmacokinetics

Abstract

Combinations of the direct renin inhibitor aliskiren with angiotensin receptor blockers (ARBs) or diuretics are effective therapeutic regimens for the treatment of hypertension. A large database of safety information has become available during the past several years with aliskiren in combination trials. Data were pooled from 9 short-term (8-week) and 4 longer-term (26- to 52-week) randomized controlled trials of aliskiren in patients with hypertension. Adverse event (AE) rates were assessed for aliskiren combination therapy compared with component monotherapies. In short-term studies, overall AE rates were similar for patients receiving aliskiren/valsartan or aliskiren/diuretic combinations (32.2%-39.8%) and those receiving the component monotherapies (30.0%-39.6%). In longer-term studies, AE rates with aliskiren/losartan (55.5%) and aliskiren/diuretic (45.0%) combination therapy were similar to those with losartan (53.9%) and diuretic (48.9%) alone. Angioedema and hyperkalemia occurred in similar proportions of patients taking combination therapies vs monotherapy. The safety and tolerability profile of aliskiren in combination with the ARBs valsartan or losartan, or diuretic, is similar to aliskiren, ARBs, or diuretics alone., (© 2011 Wiley Periodicals, Inc.)

Published

2011

84. What to do with refractory urticaria patients.

Author

Kaplan AP

Subjects

Humans, Urticaria etiology, Urticaria metabolism, Urticaria pathology, Urticaria drug therapy

Published

2011

85. Omalizumab is effective in nonautoimmune urticaria.

Author

Ferrer M, Gamboa P, Sanz ML, Goikoetxea MJ, Cabrera-Freitag P, Javaloyes G, Berroa F, and Kaplan AP

Subjects

Adult, Anti-Allergic Agents administration & dosage, Antibodies, Anti-Idiotypic administration & dosage, Antibodies, Monoclonal administration & dosage, Antibodies, Monoclonal, Humanized, Chronic Disease, Drug Administration Schedule, Female, Humans, Male, Middle Aged, Omalizumab, Severity of Illness Index, Treatment Outcome, Urticaria physiopathology, Young Adult, Anti-Allergic Agents therapeutic use, Antibodies, Anti-Idiotypic therapeutic use, Antibodies, Monoclonal therapeutic use, Urticaria drug therapy

Published

2011

86. Bradykinin and the pathogenesis of hereditary angioedema.

Author

Kaplan AP

Published

2011

87. Unmet clinical needs in chronic spontaneous urticaria. A GA²LEN task force report.

Author

Maurer M, Weller K, Bindslev-Jensen C, Giménez-Arnau A, Bousquet PJ, Bousquet J, Canonica GW, Church MK, Godse KV, Grattan CE, Greaves MW, Hide M, Kalogeromitros D, Kaplan AP, Saini SS, Zhu XJ, and Zuberbier T

Subjects

Advisory Committees, Chronic Disease, Humans, Prevalence, Quality of Life, Stress, Psychological, Urticaria diagnosis, Urticaria epidemiology, Urticaria therapy

Abstract

Chronic spontaneous urticaria, formerly also known as chronic idiopathic urticaria and chronic urticaria (CU), is more common than previously thought. At any time, 0.5-1% of the population suffers from the disease (point prevalence). Although all age groups can be affected, the peak incidence is seen between 20 and 40 years of age. The duration of the disease is generally 1-5 years but is likely to be longer in more severe cases, cases with concurrent angioedema, in combination with physical urticaria or with a positive autologous serum skin test (autoreactivity). Chronic spontaneous urticaria has major detrimental effects on quality of life, with sleep deprivation and psychiatric comorbidity being frequent. It also has a large impact on society in terms of direct and indirect health care costs as well as reduced performance at work and in private life. In the majority of patients, an underlying cause cannot be identified making a causal and/or curative treatment difficult. Nonsedating H₁-antihistamines are the mainstay of symptomatic therapy, but treatment with licensed doses relieves symptoms effectively in < 50% of patients. Although guideline-recommended updosing up to fourfold increases symptom control in many patients, a substantial number of patients have only little benefit from H₁ -antihistamines. Consequently, there is a great need for new therapeutic strategies., (© 2010 John Wiley & Sons A/S.)

Published

2011

88. Stimulated neuronal expression of brain-derived neurotrophic factor by Neurotropin.

Author

Fukuda Y, Berry TL, Nelson M, Hunter CL, Fukuhara K, Imai H, Ito S, Granholm-Bentley AC, Kaplan AP, and Mutoh T

Subjects

Animals, Behavior, Animal drug effects, Brain-Derived Neurotrophic Factor genetics, Cyclic AMP Response Element-Binding Protein metabolism, Down Syndrome metabolism, Hippocampus cytology, Hippocampus metabolism, Humans, Male, Memory drug effects, Mice, Mitogen-Activated Protein Kinases metabolism, Neuroblastoma metabolism, Neurons cytology, Rabbits, Receptor, trkB metabolism, Tumor Cells, Cultured, Adjuvants, Immunologic pharmacology, Brain-Derived Neurotrophic Factor metabolism, Neurons drug effects, Neurons metabolism, Polysaccharides pharmacology

Abstract

Expression of brain-derived neurotrophic factor (BDNF) was stimulated in human neuroblastoma SH-SY5Y cells by a nonprotein extract of inflamed rabbit skin inoculated with vaccinia virus (Neurotropin), an analgesic widely used in Japan for treatment of disorders associated with chronic pain, with the optimal dosage at 10mNU/mL. This stimulation was accompanied by activations of p42/44 MAP kinase, CREB and c-Fos expression. Inhibitors of MAP kinases or PI 3-kinase prevented the stimulatory action of Neurotropin, indicating that neuronal TrkB/CREB pathway mediates the action. Repetitive oral administration of Neurotropin (200NU/kg/day, 3months) prevented the age-dependent decline in hippocampal BDNF expression in Ts65Dn mice, a model of Down's syndrome. This effect was associated with the improvement of spatial cognition of the mice. These results open an intriguing new strategy in which Neurotropin may prove beneficial treatment for neurodegenerative disorders., (Copyright © 2010 Elsevier Inc. All rights reserved.)

Published

2010

89. Enzymatic pathways in the pathogenesis of hereditary angioedema: the role of C1 inhibitor therapy.

Author

Kaplan AP

Subjects

Humans, Angioedemas, Hereditary drug therapy, Angioedemas, Hereditary enzymology, Angioedemas, Hereditary physiopathology, Complement C1 Inhibitor Protein metabolism, Complement C1 Inhibitor Protein therapeutic use

Abstract

A functional abnormality of C1 inhibitor (C1INH) is present in types I and II hereditary angioedema (HAE), and normal C1INH may be rendered ineffective in the newly described type III HAE. C1INH inhibits factor XIIa, factor XII fragment (XIIf), kallikrein, and plasmin. Thus, in its absence, there is marked activation of the bradykinin-forming cascade resulting in severe angioedema. Factor XII may autoactivate on binding to endothelial cell surface gC1qR (receptor for the globular heads of C1q) thus initiating the cascade. Alternatively, stimuli that activate endothelial cells may liberate (or express at the cell surface) heat shock protein 90 or the enzyme prolylcarboxypeptidase, either of which can interact with the prekallikrein-high-molecular-weight kininogen complex to convert prekallikrein to kallikrein stoichiometrically. The kallikrein produced can cleave high-molecular-weight kininogen to produce bradykinin and also recruit factor XII by enzymatically activating it. Patients with type I or II HAE have mutant C1INH so that control of C1 activation is lost. Autoactivation of C1r in the absence of C1INH leads to C1s activation followed by C4 cleavage and depletion. An attack of swelling is accompanied by conversion of factor XIIa to factor XIIf and further enzymatic activation of C1r so that C4 levels drop further and C2 is depleted. New therapies for HAE focus on the bradykinin-forming cascade and include a kallikrein inhibitor and a bradykinin B-2 receptor antagonist in addition to administration of purified C1INH., (Copyright © 2010 American Academy of Allergy, Asthma & Immunology. Published by Mosby, Inc. All rights reserved.)

Published

2010

90. Safety and tolerability of the direct renin inhibitor aliskiren: a pooled analysis of clinical experience in more than 12,000 patients with hypertension.

Author

White WB, Bresalier R, Kaplan AP, Palmer BF, Riddell RH, Lesogor A, Chang W, and Keefe DL

Subjects

Aged, Amides therapeutic use, Antihypertensive Agents therapeutic use, Female, Fumarates therapeutic use, Humans, Incidence, Male, Middle Aged, Renin-Angiotensin System drug effects, Risk, Amides adverse effects, Antihypertensive Agents adverse effects, Fumarates adverse effects, Hypertension drug therapy, Renin antagonists & inhibitors

Abstract

While the safety of renin-angiotensin system (RAS)-blocking drugs such as angiotensin-converting enzyme (ACE) inhibitors and angiotensin receptor blockers is well known, less is known about the new direct renin inhibitor aliskiren. The authors pooled data from 12 randomized controlled trials of aliskiren in patients with hypertension and analyzed the incidence and types of adverse events (AEs) and laboratory abnormalities. Studies were characterized as short-term (≤2 months) placebo-controlled or long-term (>2 months) active-controlled. Relative risks for AEs of particular interest for RAS blockers were calculated. In short-term studies, AEs occurred in similar proportions of aliskiren 150 mg and 300 mg (33.6% and 31.6%, respectively) and placebo treatment groups (36.8%). In long-term studies, a lower proportion of patients treated with aliskiren 150 mg and 300 mg had AEs (33.7% and 43.2%, respectively) than those treated with ACE inhibitors (60.1%), angiotensin receptor blockers (53.9%), and thiazide diuretics (48.9%). Events of special interest, including angioedema, hyperkalemia, and diarrhea occurred in similar proportions of patients taking aliskiren, placebo, and comparator agents. In studies of up to 36 weeks, patients treated with aliskiren were significantly less likely to develop cough than those treated with ACE inhibitors. At the registered doses of 150 mg and 300 mg daily, aliskiren has safety and tolerability profiles similar to placebo, other RAS blockers, and diuretics. Cough rates are lower with aliskiren compared with ACE inhibitors., (© 2010 Wiley Periodicals, Inc.)

Published

2010

91. The plasma bradykinin-forming pathways and its interrelationships with complement.

Author

Kaplan AP and Ghebrehiwet B

Subjects

Animals, Bradykinin blood, Complement C1 Inhibitor Protein metabolism, Complement System Proteins metabolism, Factor XII metabolism, Humans, Kallikreins metabolism, Kininogen, High-Molecular-Weight metabolism, Biosynthetic Pathways, Bradykinin biosynthesis, Complement Activation immunology, Complement System Proteins immunology

Abstract

The plasma bradykinin-forming cascade and the complement pathways share many elements, including cross-activation, common control mechanisms, and shared binding proteins. The C1 inhibitor (C1 INH) is not only the inhibitor of activated C1r and C1s, but it is the key control protein of the plasma bradykinin-forming cascade. It inhibits the autoactivation of Factor XII, the ability of Factor XIIa to activate prekallikrein and Factor XI, the activation of high molecular weight kininogen (HK) by kallikrein, and the feedback activation of Factor XII by kallikrein. Thus in the absence of C1 INH (hereditary angioedema or acquired C1 INH deficiency) there is unimpeded formation of bradykinin leading to angioedema. Activated Factor XII (Factor XIIa, 80,000 kDa) is further cleaved by kallikrein or plasmin to yield Factor XII fragment (Factor XIIf, 30,000 kDa) and Factor XIIf can activate the C1r subcomponent of C1, particularly when C1 INH (which inhibits Factor XIIf) is absent. Once bradykinin is formed, it causes vasodilatation and increased vascular permeability by interaction with constitutively expressed B-2 receptors. However degradation of bradykinin by carboxypeptidase N (in plasma) or carboxypeptidase M (on endothelial cells) yields des-arg-9 (Kerbiriou and Griffin, 1979) bradykinin which interacts with B-1 receptors. B-1 receptors are induced in inflammatory states by cytokines such as Interleukin 1 and its interaction with bradykinin may prolong or perpetuate the vascular response until bradykinin is completely inactivated by angiotensin converting enzyme or aminopeptidase P, or neutral endopeptidase. The entire bradykinin-forming cascade is assembled and can be activated along the surface of endothelial cells in zinc dependent reactions involving gC1qR, cytokeratin 1, and the urokinase plasminogen activated receptor (u-PAR). Although Factors XII and HK can be shown to bind to each one of these proteins, they exist in endothelial cells as two bimolecular complexes; gC1qR-cytokeratin 1, which preferentially binds HK, and cytokeratin 1-u-PAR which preferentially binds Factor XII. The gC1qR, which binds the globular heads of C1q is present in excess and can bind either Factor XII or HK however the binding sites for HK and C1q have been shown to reside at opposite ends of gC1qR. Activation of the bradykinin-forming pathway can be initiated at the cell surface by gC1qR-induced autoactivation of Factor XII or direct activation of the prekallikrein-HK complex by endothelial cell-derived heat-shock protein 90 (HSP 90) or prolylcarboxypeptidase with recruitment or Factor XII by the kallikrein produced., (Copyright 2010 Elsevier Ltd. All rights reserved.)

Published

2010

92. Treatment of cold urticaria.

Author

Kaplan AP

Published

2010

93. Dietary therapy for chronic urticaria.

Author

Kaplan AP

Published

2010

94. Kinin formation in C1 inhibitor deficiency.

Author

Kaplan AP and Joseph K

Subjects

Angioedemas, Hereditary pathology, Angioedemas, Hereditary physiopathology, Animals, Bradykinin analogs & derivatives, Bradykinin pharmacology, Capillary Permeability drug effects, Complement C1 Inhibitor Protein metabolism, Epithelial Cells drug effects, Epithelial Cells immunology, Epithelial Cells pathology, Humans, Rats, Receptor, Bradykinin B1 agonists, Vasodilator Agents pharmacology, Angioedemas, Hereditary drug therapy, Bradykinin therapeutic use, Complement C1 Inhibitor Protein genetics, Epithelial Cells metabolism

Published

2010

95. The bradykinin-forming cascade and its role in hereditary angioedema.

Author

Kaplan AP and Joseph K

Subjects

Androgens therapeutic use, Angioedemas, Hereditary drug therapy, Complement C1 Inactivator Proteins therapeutic use, Complement Inactivating Agents therapeutic use, Endothelial Cells metabolism, Factor XII metabolism, HSP90 Heat-Shock Proteins metabolism, Humans, Kallikreins antagonists & inhibitors, Kallikreins metabolism, Kininogen, High-Molecular-Weight metabolism, Plasma Kallikrein metabolism, Prekallikrein metabolism, Receptor, Bradykinin B2 metabolism, Angioedemas, Hereditary metabolism, Bradykinin metabolism

Abstract

Objective: To review the mechanisms by which bradykinin is generated in hereditary angioedema (HAE) (C1 inhibitor deficiency), including the role of human plasma proteins and endothelial cells., Data Sources: Published articles in reviewed journals that address (1) the fundamentals of bradykinin formation, (2) interactions between kinin-forming proteins and endothelial cells, (3) clinical evidence that bradykinin causes swelling in HAE, and (4) therapeutic options focused on inhibition of the plasma kallikrein-kinin cascade., Study Selection: Historical articles that have made fundamental observations. Recent articles that address evolving concepts of disease pathogenesis and treatment., Results: C1 inhibitor deficiency causes dysregulation of the plasma bradykinin-forming cascade with overproduction of bradykinin due to uninhibited effects of activated factor XII and plasma kallikrein. Swelling in HAE and production of bradykinin are localized (and may then disseminate); activation along the endothelial cell surface involves cell membrane ligands of factor XII and high-molecular-weight kininogen, release of endothelial cell heat shock protein 90, activation of the high-molecular-weight kininogen-prekallikrein complex, and endothelial cell activation at the B2 receptor. Attacks of swelling may be terminated by treatment with a kallikrein inhibitor or B2 receptor blockade. Replenishing C1 inhibitor can abort attacks of swelling and provide prophylaxis with intravenous administration., Conclusions: Bradykinin is the mediator of swelling in types I and II HAE and is overproduced because of a deficiency in C1 inhibitor. Inhibition of bradykinin formation by novel agentscan provide targeted therapeutic approaches that address the pathophysiologic abnormalities.

Published

2010

96. Kinins, airway obstruction, and anaphylaxis.

Author

Kaplan AP

Subjects

Airway Obstruction etiology, Anaphylaxis blood, Anaphylaxis physiopathology, Angiotensin-Converting Enzyme Inhibitors adverse effects, Animals, Blood Coagulation, Complement System Proteins deficiency, Factor XIa immunology, Humans, Kinins metabolism, Anaphylaxis immunology, Complement System Proteins immunology, Endothelial Cells immunology, Kinins immunology

Abstract

Anaphylaxis is a term that implies symptoms that are present in many organs, some of which are potentially fatal. The pathogenic process can either be IgE-dependent or non-IgE-dependent; the latter circumstance may be referred to as anaphylactoid. Bradykinin is frequently responsible for the manifestations of IgE-independent reactions. Blood levels may increase because of overproduction; diseases such as the various forms of C1 inhibitor deficiency (hereditary or acquired) or hereditary angioedema with normal C1 inhibitor are examples in this category. Blood levels may also increase because of an abnormality in bradykinin metabolism; the angioedema due to ACE inhibitors is a commonly encountered example. Angioedema due to bradykinin has the potential to cause airway obstruction and asphyxia as well as severe gastrointestinal symptoms simulating an acute abdomen. Formation of bradykinin in plasma is a result of a complex interaction among proteins such as factor XII, prekallikrein, and high molecular weight kininogen (HK) resulting in HK cleavage and liberation of bradykinin. These proteins also assemble along the surface of endothelial cells via zinc-dependent interactions with gC1qR, cytokeratin 1, and u-PAR. Endothelial cell expression (or secretion) of heat-shock protein 90 or prolylcarboxypeptidase can activate the prekallikrein-HK complex to generate bradykinin in the absence of factor XII, however factor XII is then secondarily activated by the kallikrein that results. Bradykinin is destroyed by carboxypeptidase N and angiotensin-converting enzyme. The hypotension associated with IgE-dependent anaphylaxis maybe mediated, in part, by massive proteolytic digestion of HK by kallikreins (tissue or plasma-derived) or other cell-derived kininogenases., (Copyright 2010 S. Karger AG, Basel.)

Published

2010

97. Treatment of episodes of hereditary angioedema with C1 inhibitor: serial assessment of observed abnormalities of the plasma bradykinin-forming pathway and fibrinolysis.

Author

Joseph K, Tholanikunnel TE, and Kaplan AP

Subjects

Angioedemas, Hereditary blood, Angioedemas, Hereditary genetics, Angioedemas, Hereditary physiopathology, Bradykinin antagonists & inhibitors, Bradykinin blood, Bradykinin genetics, Complement Activation drug effects, Complement C1 Inhibitor Protein genetics, Complement C1 Inhibitor Protein immunology, Complement C4a metabolism, Factor XIIa metabolism, Fibrinolysin metabolism, Fibrinolysin pharmacology, Fibrinolysis genetics, Fibrinolysis immunology, Humans, Infusions, Intravenous, Kallikreins blood, Kallikreins pharmacology, Mutation, Angioedemas, Hereditary drug therapy, Bradykinin biosynthesis, Complement C1 Inhibitor Protein metabolism, Complement C1 Inhibitor Protein pharmacology, Fibrinolysis drug effects

Abstract

Background: Hereditary angioedema (HAE) is typically the result of a deficiency of C1 inhibitor (C1-INH) with gene defects that lead to diminished plasma levels or the production of a dysfunctional protein. Replacement therapy with C1-INH has been shown to be effective in ameliorating episodes of swelling. We have reported elevated baseline levels of bradykinin, C4a, and plasmin-alpha2-antiplasmin complexes in the plasma of patients with HAE compared with the plasma of healthy controls. The production of factor XII fragment on in vitro activation of plasma with HAE has also been observed., Objective: To perform serial assessment of abnormalities of the bradykinin-forming pathway and fibrinolysis in patients with HAE after treatment of episodes of swelling with intravenous C1-INH., Methods: We obtained samples of plasma from 9 patients with HAE at a quiescent period (baseline), during an attack of swelling, and at 1, 4, and 12 hours after termination of an infusion of C1-INH. Factor XIIa, kallikrein, and plasmin were each measured by cleavage of synthetic substrates specific for each item., Results: Each enzyme was strikingly elevated at baseline compared with the levels in pooled healthy plasma, and there was a progressive decline of activity to normal for factor XIIa and plasmin. Kallikrein decreased in 7 of the 9 patients at 1 hour and then decreased in all patients. Bradykinin levels were elevated at the outset in all patients, increased prominently during an attack of swelling, decreased to baseline after 1 hour, and then decreased toward normal by 4 and 12 hours., Conclusion: The plasma levels of factor XIIa, kallikrein, and bradykinin decreased when measured serially subsequent to the infusion of nanofiltered C1-INH.

Published

2010

98. Factor XII-independent cleavage of high-molecular-weight kininogen by prekallikrein and inhibition by C1 inhibitor.

Author

Joseph K, Tholanikunnel BG, and Kaplan AP

Subjects

Blotting, Western, Bradykinin chemistry, Catalysis, Electrophoresis, Polyacrylamide Gel, Humans, Prekallikrein antagonists & inhibitors, Prekallikrein chemistry, Complement C1 Inhibitor Protein metabolism, Factor XII chemistry, Kininogen, High-Molecular-Weight chemistry, Kininogen, High-Molecular-Weight metabolism, Prekallikrein metabolism

Abstract

Background: Bradykinin formation typically requires interaction of Factor XII, prekallikrein (PK), and high-molecular-weight kininogen (HK) with negatively charged exogenous initiators or cell-surface proteins. Approximately 85% of plasma PK circulates as a complex with HK. Nonenzymatic cell-derived initiators, such as heat shock protein 90, can activate the HK-PK complex to generate kallikrein, bradykinin, and cleaved HK, even in the absence of Factor XII., Objective: We sought to determine whether PK, without activation to kallikrein, can digest HK to release bradykinin., Methods: Kallikrein was measured by using a chromogenic assay, and bradykinin levels were determined by ELISA. Cleavage of PK and HK were assessed by SDS-PAGE and Western blot analysis., Results: Cleavage of HK by PK is demonstrated without any conversion of PK to kallikrein. HK cleavage by PK is distinguished from that of kallikrein by the following: (1) stoichiometric activation of HK by PK with release of bradykinin proportional to the PK input; (2) inhibition of PK cleavage of HK by corn trypsin inhibitor, which has no effect on kallikrein; and (3) inhibition of PK cleavage of HK by a peptide derived from HK, which inhibits binding of PK to HK. The same peptide has no effect on kallikrein activation of HK. C1 inhibitor (C1INH), the major control protein of the plasma bradykinin-forming cascade, inhibits PK cleavage of HK., Conclusion: PK is an enzyme that can cleave HK to release bradykinin, and this reaction is inhibited by C1INH. This might account, in part, for circulating bradykinin levels and initiation of kinin formation in C1INH deficiency.

Published

2009

99. Pathogenesis of chronic urticaria.

Author

Kaplan AP and Greaves M

Subjects

Antibodies, Anti-Idiotypic immunology, Antibodies, Anti-Idiotypic metabolism, Autoimmunity, Basophils metabolism, Cell Degranulation immunology, Chronic Disease, Histamine immunology, Histamine metabolism, Humans, Immunoglobulin E blood, Mast Cells metabolism, Skin immunology, Skin pathology, Thyroglobulin immunology, Thyroglobulin metabolism, Thyroid Gland immunology, Thyroid Gland metabolism, Autoantibodies blood, Basophils immunology, Mast Cells immunology, Urticaria immunology, Urticaria pathology

Abstract

Chronic urticaria is defined as the presence of urticaria (hives) for at least 6 weeks with the assumption that it occurs daily or close to it. If we eliminate physical urticarias and urticarial vasculitis from consideration, the remainder can be divided into autoimmune chronic urticaria (45%) and idiopathic chronic urticaria (55%). The autoimmune subgroup is associated with the IgG anti-IgE receptor alpha subunit in 35-40% of patients and IgG anti-IgE in an additional 5-10%. These autoantibodies have been shown to activate blood basophils and cutaneous mast cells in vitro with augmentation of basophil activation by complement and release of C5a, in particular. Binding methods (immunoblot and ELISA) yield positives in many autoimmune diseases as well as occasional normal subjects or patients with other forms of urticaria but most such sera are non-functional. Activation of basophils or mast cells causing histamine release is quite specific for chronic urticaria and defines the autoimmune subgroup. Although pathogenicity is not formally proven, the antibodies cause wealing upon intradermal injection, and removal of the autoantibody leads to remission. A cellular infiltrate is seen to be characterized by mast cell degranulation and infiltration of CD4+ T lymphocytes, monocytes, neutrophils, eosinophils, and basophils. The intensity of the infiltrate and clinical severity of the disease (including accompanying angio-oedema) is more severe in the autoimmune subpopulation. This latter group also has a higher evidence of human leucocyte antigen DR alleles associated with autoimmunity and a 25% incidence of antithyroid antibodies with diagnosed hypothyroidism in some. Hypo-responsiveness of patients' basophils to anti-IgE and hyperresponsiveness to serum defines another subpopulation (at least 50%) that overlaps the idiopathic and autoimmune subgroups. Hypo-responsiveness to anti-IgE has been shown to be associated with elevated levels of cytoplasmic phosphatases that inhibit degranulation. Reversal of the abnormality is seen with disease remission. Further work will be needed to distinguish whether this is a cause or a consequence of persistent urticaria and to further assess the relationship (or lack thereof) of altered responsiveness (decreased or increased) with the presence or absence of activating autoantibodies.

Published

2009

100. What the first 10,000 patients with chronic urticaria have taught me: a personal journey.

Author

Kaplan AP

Subjects

Allergens immunology, Autoantibodies blood, Autoimmunity, Chronic Disease, Cyclosporine administration & dosage, Guidelines as Topic, Histamine Antagonists administration & dosage, Humans, Hydroxyzine administration & dosage, Immunosuppressive Agents administration & dosage, Methotrexate administration & dosage, Urticaria immunology, Urticaria pathology, Cyclosporine therapeutic use, Histamine Antagonists therapeutic use, Hydroxyzine therapeutic use, Immunosuppressive Agents therapeutic use, Methotrexate therapeutic use, Urticaria drug therapy

Published

2009