Your search keyword '"López-Lera A"' showing total 40 results

1. Altered levels of phospholipases C, diacylglycerols, endocannabinoids, and N-acylethanolamines in patients with hereditary angioedema due to FXII mutation.

Author

Ferrara AL, Palestra F, Piscitelli F, Petraroli A, Suffritti C, Firinu D, López-Lera A, Caballero T, Bork K, Spadaro G, Marone G, Di Marzo V, Bova M, and Loffredo S

Abstract

Background: Hereditary angioedema (HAE) is a rare genetic disorder characterized by local, self-limiting edema due to temporary increase in vascular permeability. HAE with normal C1 esterase inhibitor (C1INH) activity includes the form with mutations in the F12 gene encoding for coagulation factor XII (FXII-HAE) causing an overproduction of bradykinin (BK) leading to angioedema attack. BK binding to B2 receptors (BK2R) leads to an activation of phospholipase C (PLC) and subsequent generation of second messengers: diacylglycerols (DAGs) and possibly the endocannabinoids (eCBs), 2-arachidonoylglycerol (2-AG) and anandamide (AEA), and eCB-related N-acylethanolamines [palmitoylethanolamide (PEA) and oleoylethanolamide (OEA)]. To date, there are no data on the role of these lipid mediators in FXII-HAE., Methods: Here, we analyzed plasma levels of PLC, DAGs, and eCBs in 40 patients with FXII-HAE and 40 sex- and age-matched healthy individuals., Results: Plasma PLC activity was increased in FXII-HAE patients compared to controls. Concentrations of DAG 18:1-20:4, a lipid second messenger produced by PLC, were higher in FXII-HAE compared to controls, and positively correlated with PLC activity and cleaved high molecular kininogen (cHK). Also the concentrations of the DAG metabolite, 2-AG were altered in FXII-HAE. AEA and OEA were decreased in FXII-HAE patients compared to controls; by contrast, PEA, was increased. The levels of all tested mediators did not differ between symptomatic and asymptomatic patients. Moreover, C1INH-HAE patients had elevated plasma levels of PLC, which correlated with cHK, but the levels of DAGs and eCBs were the same as controls., Conclusions: BK overproduction and BKR2 activation are linked to alteration of PLCs and their metabolites in patients with FXII-HAE. Our results may pave way to investigations on the functions of these mediators in the pathophysiology of FXII-HAE, and provide new potential biomarkers and therapeutic targets., (© 2024 European Academy of Allergy and Clinical Immunology and John Wiley & Sons Ltd.)

Published

2024

2. Inherited Human BCL10 Deficiencies.

Author

Alsaidalani AA, García-Solís B, Bukhari E, Van Den Rym A, López-Collazo E, Sánchez-Ramón S, Corvillo F, López-Lera A, de Andrés A, Martínez-Barricarte R, and Perez de Diego R

Subjects

Humans, B-Cell CLL-Lymphoma 10 Protein genetics, Bone Marrow Transplantation, Mutation genetics, Immunologic Deficiency Syndromes diagnosis, Immunologic Deficiency Syndromes genetics, Immunologic Deficiency Syndromes therapy

Abstract

Human BCL10 deficiency causes combined immunodeficiency with bone marrow transplantation as its only curative option. To date, there are four homozygous mutations described in the literature that were identified in four unrelated patients. Here, we describe a fifth patient with a novel mutation and summarize what we have learned about BCL10 deficiency. Due to the severity of the disease, accurate knowledge of its clinical and immunological characteristics is instrumental for early diagnosis and adequate clinical management of the patients., (© 2023. The Author(s), under exclusive licence to Springer Science+Business Media, LLC, part of Springer Nature.)

Published

2023

3. Properdin deficiency associated with systemic meningococcal disease due to a novel p.Cys337Arg pathogenic variant.

Author

González-Sánchez L, Agudo AM, Van Den Rym A, Begiristain MI, Saizar A, Pérez de Diego R, Nozal P, López-Lera A, López-Trascasa M, and Corvillo F

Published

2023

4. Inherited human ezrin deficiency impairs adaptive immunity.

Author

García-Solís B, Van Den Rym A, Martinez-Martínez L, Franco T, Pérez-Caraballo JJ, Markle J, Cubillos-Zapata C, Marín AV, Recio MJ, Regueiro JR, Navarro-Zapata A, Mestre-Durán C, Ferreras C, Martín Cotázar C, Mena R, de la Calle-Fabregat C, López-Lera A, Fernández Arquero M, Pérez-Martínez A, López-Collazo E, Sánchez-Ramón S, Casanova JL, Martínez-Barricarte R, de la Calle-Martín O, and Pérez de Diego R

Subjects

Humans, Cell Membrane metabolism, Immunity, Humoral, CD8-Positive T-Lymphocytes, Cytoskeleton metabolism

Abstract

Background: Inborn errors of immunity (IEI) are a group of monogenic diseases that confer susceptibility to infection, autoimmunity, and cancer. Despite the life-threatening consequences of some IEI, their genetic cause remains unknown in many patients., Objective: We investigated a patient with an IEI of unknown genetic etiology., Methods: Whole-exome sequencing identified a homozygous missense mutation of the gene encoding ezrin (EZR), substituting a threonine for an alanine at position 129., Results: Ezrin is one of the subunits of the ezrin, radixin, and moesin (ERM) complex. The ERM complex links the plasma membrane to the cytoskeleton and is crucial for the assembly of an efficient immune response. The A129T mutation abolishes basal phosphorylation and decreases calcium signaling, leading to complete loss of function. Consistent with the pleiotropic function of ezrin in myriad immune cells, multidimensional immunophenotyping by mass and flow cytometry revealed that in addition to hypogammaglobulinemia, the patient had low frequencies of switched memory B cells, CD4 + and CD8 + T cells, MAIT, γδ T cells, and central naive CD4 + cells., Conclusions: Autosomal-recessive human ezrin deficiency is a newly recognized genetic cause of B-cell deficiency affecting cellular and humoral immunity., (Copyright © 2023 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2023

5. Characterization and Clinical Association of Autoantibodies Against Perilipin 1 in Patients With Acquired Generalized Lipodystrophy.

Author

Corvillo F, Abel BS, López-Lera A, Ceccarini G, Magno S, Santini F, Araújo-Vilar D, Brown RJ, Nozal P, and López-Trascasa M

Subjects

Humans, Perilipin-1 metabolism, Autoantibodies metabolism, Immunoglobulin G metabolism, 1-Acylglycerol-3-Phosphate O-Acyltransferase metabolism, Lipodystrophy, Congenital Generalized complications, Lipodystrophy metabolism

Abstract

Acquired generalized lipodystrophy (AGL) is a rare condition characterized by massive loss of adipose tissue through the body, causing severe metabolic complications. Autoimmune destruction of adipocytes is strongly suspected based on the frequent association of AGL with autoimmune disorders. In 2018, autoantibodies against perilipin 1 (PLIN1) were identified in three patients with autoimmune-associated AGL. However, the pathogenic mechanism and clinical impact of anti-PLIN1 remain unsolved. The prevalence of anti-PLIN1 autoantibodies in an AGL cohort of 40 patients was 50% (20 of 40). Among positive patients, 10 had the autoimmune variety and 10 had panniculitis-associated AGL. The IgG isotype was predominant, although some IgM antibodies were detected. Epitope-mapping studies did not identify a single, major epitope. Instead, autoantibodies typically bound to several different peptides, among which the central (233-405) domain was detected in all antibody-positive patients, for both IgG and IgM autoantibodies. In-depth epitope mapping indicated that anti-PLIN1 autoantibodies predominantly recognize the αβ-hydrolase domain containing 5 (ABHD5) binding site (383-405). Autoantibodies dose-dependently blocked the binding of PLIN1 to ABHD5 and caused a dislocation of ABHD5 toward the cytosol, leading to an increase in lipolysis and lipase activities. Finally, anti-PLIN1 titers significantly correlated with the amount of fat loss, metabolic control impairment, and severity of liver injury. Our data strongly support that anti-PLIN1 autoantibodies are a diagnostic biomarker and a cause of lipodystrophy in patients with AGL., (© 2022 by the American Diabetes Association.)

Published

2023

6. SERPING1 Variants and C1-INH Biological Function: A Close Relationship With C1-INH-HAE.

Author

Drouet C, López-Lera A, Ghannam A, López-Trascasa M, Cichon S, Ponard D, Parsopoulou F, Grombirikova H, Freiberger T, Rijavec M, Veronez CL, Pesquero JB, and Germenis AE

Abstract

Hereditary angioedema with C1 Inhibitor deficiency (C1-INH-HAE) is caused by a constellation of variants of the SERPING1 gene ( n = 809; 1,494 pedigrees), accounting for 86.8% of HAE families, showing a pronounced mutagenic liability of SERPING1 and pertaining to 5.6% de novo variants. C1-INH is the major control serpin of the kallikrein-kinin system (KKS). In addition, C1-INH controls complement C1 and plasminogen activation, both systems contributing to inflammation. Recognizing the failed control of C1s protease or KKS provides the diagnosis of C1-INH-HAE. SERPING1 variants usually behave in an autosomal-dominant character with an incomplete penetrance and a low prevalence. A great majority of variants (809/893; 90.5%) that were introduced into online database have been considered as pathogenic/likely pathogenic. Haploinsufficiency is a common feature in C1-INH-HAE where a dominant-negative variant product impacts the wild-type allele and renders it inactive. Small (36.2%) and large (8.3%) deletions/duplications are common, with exon 4 as the most affected one. Point substitutions with missense variants (32.2%) are of interest for the serpin structure-function relationship. Canonical splice sites can be affected by variants within introns and exons also (14.3%). For noncanonical sequences, exon skipping has been confirmed by splicing analyses of patients' blood-derived RNAs ( n = 25). Exonic variants ( n = 6) can affect exon splicing. Rare deep-intron variants ( n = 6), putatively acting as pseudo-exon activating mutations, have been characterized as pathogenic. Some variants have been characterized as benign/likely benign/of uncertain significance ( n = 74). This category includes some homozygous ( n = 10) or compound heterozygous variants ( n = 11). They are presenting with minor allele frequency (MAF) below 0.00002 (i.e., lower than C1-INH-HAE frequency), and may be quantitatively unable to cause haploinsufficiency. Rare benign variants could contribute as disease modifiers. Gonadal mosaicism in C1-INH-HAE is rare and must be distinguished from a de novo variant. Situations with paternal or maternal disomy have been recorded ( n = 3). Genotypes must be interpreted with biological investigation fitting with C1-INH expression and typing. Any SERPING1 variant reminiscent of the dysfunctional phenotype of serpin with multimerization or latency should be identified as serpinopathy., Competing Interests: AGh was employed by KininX SAS. FP and AGe were employed by CeMIA SA. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2022 Drouet, López-Lera, Ghannam, López-Trascasa, Cichon, Ponard, Parsopoulou, Grombirikova, Freiberger, Rijavec, Veronez, Pesquero and Germenis.)

Published

2022

7. In Search of an Association Between Genotype and Phenotype in Hereditary Angioedema due to C1-INH Deficiency.

Author

Loli-Ausejo D, López-Lera A, Drouet C, Lluncor M, Phillips-Anglés E, Pedrosa M, Cabañas R, and Caballero T

Subjects

Adolescent, Complement C1 Inhibitor Protein genetics, Genetic Association Studies, Genotype, Humans, Phenotype, Angioedemas, Hereditary diagnosis, Angioedemas, Hereditary genetics

Abstract

Hereditary angioedema due to C1 inhibitor deficiency (C1-INH-HAE) is caused by mutations affecting the SERPING1 gene. Adult patients (≥ 18 years old) diagnosed with C1-INH-HAE were clustered according to a modified SERPING1 gene mutation classification [5]. Demographic, clinical, and laboratory data were studied. Published manuscripts on the genotype/phenotype relationship were reviewed. Eighty-eight patients participated in the study, with 78 having a classifiable mutation. We compared the data in the 3 largest groups: class 0 only (n = 32), class II only (n = 18), class III only (n = 22). Antigenic C4 and C1 inhibitors were higher in class II (p = 0.008 and p = 0.02, respectively), and facial attacks in the last 6 months were more frequent in class III (p = 0.04)). All the other differences were non-significant. Twelve manuscripts on phenotype/genotype correlation were found: missense mutations in SERPING1 gene were associated with delay in disease onset and lower severity score in some studies, whereas the CC F12-C46T/C polymorphism produced earlier disease onset. Our study shows minimal differences regarding clinical phenotype in patients with class 0, II, and III SERPING1 gene mutations, with a tendency to class III having a more severe phenotype. The study should be performed in a larger sample to confirm if they are significant.We propose that larger multicenter, international studies are performed, comparing different SERPING1 gene mutation classifications, combining polymorphisms in other involved genes (kallikrein-kinin system, regulation of vasculature, plasminogen activation) and using different variables and clinical scores to assess C1-INH-HAE disease activity and/or severity in order to study possible genotype/phenotype relationships., (© 2021. The Author(s), under exclusive licence to Springer Science+Business Media, LLC part of Springer Nature.)

Published

2021

8. Complement Factor D (adipsin) Levels Are Elevated in Acquired Partial Lipodystrophy (Barraquer-Simons syndrome).

Author

Corvillo F, González-Sánchez L, López-Lera A, Arjona E, Ceccarini G, Santini F, Araújo-Vilar D, Brown RJ, Villarroya J, Villarroya F, Rodríguez de Córdoba S, Caballero T, Nozal P, and López-Trascasa M

Subjects

Adolescent, Adult, Aged, Biomarkers blood, Case-Control Studies, Child, Cohort Studies, Female, Humans, Male, Middle Aged, Young Adult, Complement Factor D metabolism, Lipodystrophy blood

Abstract

Complement overactivation has been reported in most patients with Barraquer-Simons syndrome (BSS), a rare form of acquired partial lipodystrophy. Complement Factor D (FD) is a serine protease with a crucial role in the activation of the alternative pathway of the complement system, which is mainly synthesized by adipose tissue. However, its role in the pathogenesis of BSS has not been addressed. In this study, plasma FD concentration was measured in 13 patients with BSS, 20 patients with acquired generalized lipodystrophy, 22 patients with C3 glomerulopathy (C3G), and 50 healthy controls. Gene expression and immunohistochemistry studies were assayed using atrophied adipose tissue from a patient with BSS. We found significantly elevated FD levels in BSS cases compared with the remaining cohorts ( p < 0.001). There were no significant differences in FD levels between sexes but FD was strongly and directly associated with age in BSS ( r = 0.7593, p = 0.0036). A positive correlation between FD and C3 was seen in patients with C3G, characterized by decreased FD levels due to chronic C3 consumption, but no correlation was detected for BSS. Following mRNA quantification in the patient's adipose tissue, we observed decreased C FD and C3 transcript levels. In contrast, the increased FD staining detected in the atrophied areas reflects the effects of persistent tissue damage on the adipose tissue, thus providing information on the ongoing pathogenic process. Our results suggest that FD could be a reliable diagnostic biomarker involved in the pathophysiology of BSS by promoting unrestrained local complement system activation in the adipose tissue environment.C5 transcript levels. In contrast, the increased FD staining detected in the atrophied areas reflects the effects of persistent tissue damage on the adipose tissue, thus providing information on the ongoing pathogenic process. Our results suggest that FD could be a reliable diagnostic biomarker involved in the pathophysiology of BSS by promoting unrestrained local complement system activation in the adipose tissue environment.

Published

2021

9. Thrombin in the Activation of the Fluid Contact Phase in Patients with Hereditary Angioedema Carrying the F12 P.Thr309Lys Variant.

Author

López-Gálvez R, de la Morena-Barrio ME, Miñano A, Pathak M, Marcos C, Emsley J, Caballero T, López-Trascasa M, Vicente V, Corral J, and López-Lera A

Subjects

Factor XII genetics, Humans, Kallikreins, Thrombin, Angioedemas, Hereditary genetics

Abstract

Hereditary angioedema due to pathogenic FXII variants (HAE-FXII) is a rare dominant disease caused by increased activation of the plasma contact system. The most prevalent HAE-FXII variant, c.1032C > A p.Thr309Lys (FXII 309Lys ), results in a smaller FXII protein with increased sensitivity to fluid-phase activation by poorly understood mechanisms. We aimed to investigate the functionality of the FXII 309Lys variant in 33 HAE-FXII patients, 25 healthy controls and 46 patients with congenital disorders of glycosylation (CDG). Activation of the plasma contact system was assessed by western blot and amidolytic assay in basal conditions or after treatment with either artificial or physiological activators. Recombinant wild-type and FXII 309Lys variants were expressed in S2 insect (Drosophila) cells. Amidolytic and fibrin generation assays were performed in fresh plasma samples. FXII 309Lys samples exhibited an increased electrophoretic mobility comparable with N-glycan-deficient FXII from CDG patients and asialo-FXII generated by neuraminidase treatment. They presented increased sensitivity to activation by dextran sulphate and silica which resulted in the generation of an aberrant 37-kDa heavy chain. We did not observe increased susceptibility of FXII 309Lys to proteolysis by exogenous or tPA-generated plasmin. However, both exogenous and endogenous thrombin cleaved the FXII 309Lys variant, releasing a 37-kDa fragment and resulting in enhanced proteolytic activation on the fluid phase. This model supports a sequential proteolytic activation process involving thrombin priming of FXII 309Lys , followed by kallikrein cleavage and generation of active βFXIIa. The present results and the observation that angioedema episodes in HAE-FXII patients occur predominantly during hypercoagulable situations suggest a key role for thrombin., (© 2021. The Author(s), under exclusive licence to Springer Science+Business Media, LLC part of Springer Nature.)

Published

2021

10. Pathophysiology and underlying mechanisms in hereditary angioedema.

Author

López Lera A

Subjects

Angioedemas, Hereditary enzymology, Complement C1 Inhibitor Protein metabolism, Humans, Peptide Hydrolases pharmacokinetics, Angioedemas, Hereditary physiopathology, Kallikrein-Kinin System physiology

Abstract

This review aims to summarize the main pathophysiological events involved in the development of hereditary angioedema (OMIM#106100). Hereditary angioedema is a rare genetic disease inherited in an autosomal dominant manner and caused by a loss of control over the plasma contact system or kallikrein-kinin system, which results in unrestrained bradykinin generation or signaling. In patients with hereditary angioedema, BK binding to endothelial cells leads to recurrent episodes of swelling at subcutaneous or submucosal tissues that can be life threatening when affecting the upper respiratory tract. The disease can either present with hypocomplementemia owing to the presence of pathogenic variants in the gene encoding complement C1 inhibitor (hereditary angioedema with C1-inhibitor deficiency) or present with normocomplementemia and associate with elevated estrogen levels owing to gain-of-function variants in the genes encoding coagulation proteins involved in the kallikrein-kinin system (namely, coagulation FXII [FXII-associated hereditary angioedema], plasminogen [PLG-associated hereditary angioedema], and high-molecular-weight kininogen [KNG1-associated hereditary angioedema]). Moreover, in recent years, novel pathogenic variants have been described in the genes encoding angiopoietin 1 (ANGPT1-associated hereditary angioedema) and myoferlin (MYOF-associated hereditary angioedema), which further expand the pathophysiological picture of hereditary angioedema.

Published

2021

11. Evidence of ongoing complement activation on adipose tissue from an 11-year-old girl with Barraquer-Simons syndrome.

Author

Corvillo F, Nozal P, López-Lera A, De Miguel MP, Piñero-Fernández JA, De Lucas R, García-Concepción MD, Beato MJ, Araújo-Vilar D, and López-Trascasa M

Subjects

Adipose Tissue, Child, Complement Activation, Complement C3 Nephritic Factor, Female, Humans, Lipodystrophy

Abstract

Barraquer-Simons syndrome (BSS), a form of acquired partial lipodystrophy, is a rare condition characterized by gradual loss of adipose tissue from the upper body, keeping intact the white adipose tissue of the lower extremities. The etiology of BSS is not well understood, and clinical follow-up studies have not been assessed in these patients. Moreover, no histological studies have been conducted during the active phase of the disease, and complement system activation products have not been sought in the affected areas. The objective of this work was to analyze the clinical, immunological and histological events in an 11-year-old girl with BSS over a 5-year follow-up period. Clinical data were collected during six regular visits for a time period of 5 years. The circulating levels of C3, C3adesArg (a product released upon C3 activation), C4 and immunoglobulins (Ig) were quantified in serum while fat tissue from lipoatrophic areas was examined by immunohistochemical and immunofluorescence approaches. In her regular visits, no clinical or laboratory abnormalities had been observed in the patient, except for the progression of lipoatrophy linked to the C3 hypocomplementemia and the occurrence of C3 nephritic factor. Adipose tissue from the patient showed atrophied and dead adipocytes, an abnormal production of extracellular matrix, and a remarkable accumulation of infiltrating CD68 macrophages and adipocyte precursors (marked by c-Kit positiveness). Simultaneous detection of IgG, C3, C5a and C5b-9 proved the ongoing complement activity and complement-directed injury within the adipose tissue. Our results showed the first evidence that the complement system hyperactivation occurs within the adipose tissue and is linked with fat loss in patients with BSS., (© 2020 Japanese Dermatological Association.)

Published

2020

12. Factor XII in PMM2-CDG patients: role of N-glycosylation in the secretion and function of the first element of the contact pathway.

Author

López-Gálvez R, de la Morena-Barrio ME, López-Lera A, Pathak M, Miñano A, Serrano M, Borgel D, Roldán V, Vicente V, Emsley J, and Corral J

Subjects

Glycosylation, Humans, Congenital Disorders of Glycosylation genetics, Factor XII metabolism, Phosphotransferases (Phosphomutases) deficiency, Phosphotransferases (Phosphomutases) genetics

Abstract

Background: Congenital disorders of glycosylation (CDG) are rare diseases with impaired glycosylation and multiorgan disfunction, including hemostatic and inflammatory disorders. Factor XII (FXII), the first element of the contact phase, has an emerging role in hemostasia and inflammation. FXII deficiency protects against thrombosis and the p.Thr309Lys variant is involved in hereditary angioedema through the hyperreactivity caused by the associated defective O-glycosylation. We studied FXII in CDG aiming to supply further information of the glycosylation of this molecule, and its functional and clinical effects. Plasma FXII from 46 PMM2-CDG patients was evaluated by coagulometric and by Western Blot in basal conditions, treated with N-glycosydase F or activated by silica or dextran sulfate. A recombinant FXII expression model was used to validate the secretion and glycosylation of wild-type and variants targeting the two described FXII N-glycosylation sites (p.Asn230Lys; p.Asn414Lys) as well as the p.Thr309Lys variant., Results: PMM2-CDG patients had normal FXII levels (117%) but high proportions of a form lacking N-glycosylation at Asn414. Recombinant FXII p.Asn230Lys, and p.Asn230Lys&p.Asn414Lys had impaired secretion and increased intracellular retention compared to wild-type, p.Thr309Lys and p.Asn414Lys variants. The hypoglycosylated form of PMM2-CDG activated similarly than FXII fully glycosylated. Accordingly, no PMM2-CDG had angioedema. FXII levels did not associate to vascular events, but hypoglycosylated FXII, like hypoglycosylated transferrin, antithrombin and FXI levels did it., Conclusions: N-glycosylation at Asn230 is essential for FXII secretion. PMM2-CDG have high levels of FXII lacking N-glycosylation at Asn414, but this glycoform displays similar activation than fully glycosylated, explaining the absence of angioedema in CDG.

Published

2020

13. The FXII c.-4T>C Polymorphism as a Disease Modifier in Patients With Hereditary Angioedema Due to the FXII p.Thr328Lys Variant.

Author

Corvillo F, de la Morena-Barrio ME, Marcos-Bravo C, López-Trascasa M, Vicente V, Emsley J, Caballero T, Corral J, and López-Lera A

Abstract

Background: Hereditary angioedema due to the Thr328Lys variant in the coagulation factor XII (HAE-FXII) affects mainly women in whom the symptomatology is dependent on high estrogen levels. Clinical variability and incomplete penetrance are challenging features that hinder the diagnosis and management of HAE-FXII. The c.-4T>C Kozak polymorphism is the only common variation accounting for FXII plasma levels and was previously shown to modify the course of HAE due to C1-Inhibitor deficiency., Objectives: To assess the influence of the c.-4T>C polymorphism on disease expression in 39 Spanish HAE-FXII index patients., Methods: The c.-4T>C polymorphism was sequenced by the standard Sanger method, and HAE severity was calculated according to the score by Cumming et al. (2003) The activation of the contact system was quantified by the kallikrein-like activity of plasma in chromogenic assays upon activation with high-molecular-weight dextran sulfate., Results: The c.-4CC genotype was overrepresented in the studied cohort: 82% were CC-homozygous (expected frequency = 59%) and 18% were CT-heterozygous (expected frequency = 39%) ( p = 0.001). Patients with a c.-4CC genotype exhibited higher kallikrein-like activity (0.9659 ± 0.1136) than those with a c.-4TC genotype (0.7645 ± 0.1235) ( p = 0.024) or healthy donors. Moreover, the polymorphism influenced HAE-FXII severity score (c.-4CC = 4.43 ± 2.28 vs c.-4TC = 2.0 ± 1.15; p = 0.006) but not the degree of estrogen dependence or time until remission., Conclusion: The c.-4T>C polymorphism is overrepresented in a Spanish HAE-FXII cohort and significantly influences the degree of contact system activation and the clinical severity of the disease., (Copyright © 2020 Corvillo, de la Morena-Barrio, Marcos-Bravo, López-Trascasa, Vicente, Emsley, Caballero, Corral and López-Lera.)

Published

2020

14. Novel homozygous variants in the SERPING1 gene in two Turkish families with hereditary angioedema of recessive inheritance.

Author

Mete Gökmen N, Rodríguez-Alcalde C, Gülbahar O, Lopez-Trascasa M, Onay H, and López-Lera A

Subjects

Complement C1q, Complement C4, Homozygote, Humans, Turkey, Complement C1 Inhibitor Protein genetics, Hereditary Angioedema Types I and II genetics

Abstract

Hereditary angioedema as a result of deficiency of the C1 inhibitor (HAE-C1INH; MIM# 106100) is a rare autosomal disorder and affected individuals are generally heterozygous for dominant negative variants in the SERPING1 gene. Homozygosity for SERPING1 pathogenic variants was long considered to be embryonically lethal; however, five nonrelated families with a recessive HAE pattern have been described in the last decade. In this report, we functionally characterized two newly reported nonrelated, consanguineous families with a recessive presentation of HAE attributed to SERPING1 variants in the reactive center loop (family D; S438F) and gate (family A; I379T) regions. S438F heterozygotes (family D) showed variable levels of intact 105-kDa and cleaved/inactive 96-kDa isoforms of C1INH, whereas their homozygous relative presented only the 96-kDa band. Functional studies showed that S438F reduced C1INH interaction with target proteases in heterozygous (C1s, 32-38% of controls and FXIIa, 28-35% of controls) and homozygous (C1s, 18-24% of controls and FXIIa, 4-8% of controls) carriers, which is consistent with the more severe presentation of HAE in the family and decreased C1q levels in homozygous patients. By contrast, plasma C1INH from I379T heterozygotes (family A) showed normal C1INH/C1s binding (84-94% of controls) and no significant reduction in C1INH/FXIIa complexes (50-70% of controls). However, the homozygote failed to inhibit both C1s (25-42% of controls) and FXIIa (14-18% of controls). This profile is concordant with the less severe presentation of HAE in the family and the conserved C4 and C1q levels in heterozygous and homozygous patients., (© 2020 Australian and New Zealand Society for Immunology Inc.)

Published

2020

15. Correction to: Immunological features of patients affected by Barraquer-Simons syndrome.

Author

Corvillo F, Ceccarini G, Nozal P, Magno S, Pelosini C, Garrido S, López-Lera A, Moraru M, Vilches C, Fornaciari S, Gabbriellini S, Santini F, Araújo-Vilar D, and López-Trascasa M

Abstract

Following the publication of the original article [1], the authors have requested to amend the Abstract and Discussion section as follows.

Published

2020

16. Corrigendum: High Complement Factor H-Related (FHR)-3 Levels Are Associated With the Atypical Hemolytic-Uremic Syndrome-Risk Allele CFHR3 * B .

Author

Pouw RB, Gómez Delgado I, López Lera A, Rodríguez de Córdoba S, Wouters D, Kuijpers TW, and Sánchez-Corral P

Abstract

[This corrects the article DOI: 10.3389/fimmu.2018.00848.]., (Copyright © 2020 Pouw, Gómez Delgado, López Lera, Rodríguez de Córdoba, Wouters, Kuijpers and Sánchez-Corral.)

Published

2020

17. Immunological features of patients affected by Barraquer-Simons syndrome.

Author

Corvillo F, Ceccarini G, Nozal P, Magno S, Pelosini C, Garrido S, López-Lera A, Moraru M, Vilches C, Fornaciari S, Gabbriellini S, Santini F, Araújo-Vilar D, and López-Trascasa M

Subjects

Adolescent, Adult, Aged, Autoimmunity physiology, Child, Complement C3 metabolism, Complement C3 Nephritic Factor metabolism, Complement C4 metabolism, Complement Factor B metabolism, Female, Humans, Male, Middle Aged, Properdin metabolism, Young Adult, Lipodystrophy immunology, Lipodystrophy metabolism

Abstract

Background: C3 hypocomplementemia and the presence of C3 nephritic factor (C3NeF), an autoantibody causing complement system over-activation, are common features among most patients affected by Barraquer-Simons syndrome (BSS), an acquired form of partial lipodystrophy. Moreover, BSS is frequently associated with autoimmune diseases. However, the relationship between complement system dysregulation and BSS remains to be fully elucidated. The aim of this study was to provide a comprehensive immunological analysis of the complement system status, autoantibody signatures and HLA profile in BSS. Thirteen subjects with BSS were recruited for the study. The circulating levels of complement components, C3, C4, Factor B (FB) and Properdin (P), as well as an extended autoantibody profile including autoantibodies targeting complement components and regulators were assessed in serum. Additionally, HLA genotyping was carried out using DNA extracted from peripheral blood mononuclear cells., Results: C3, C4 and FB levels were significantly reduced in patients with BSS as compared with healthy subjects. C3NeF was the most frequently found autoantibody (69.2% of cases), followed by anti-C3 (38.5%), and anti-P and anti-FB (30.8% each). Clinical data showed high prevalence of autoimmune diseases (38.5%), the majority of patients (61.5%) being positive for at least one of the autoantibodies tested. The HLA allele DRB1*11 was present in 54% of BSS patients, and the majority of them (31%) were positive for *11:03 (vs 1.3% in the general population)., Conclusions: Our results confirmed the association between BSS, autoimmunity and C3 hypocomplementemia. Moreover, the finding of autoantibodies targeting complement system proteins points to complement dysregulation as a central pathological event in the development of BSS.

Published

2020

18. SERPING1 mutation update: Mutation spectrum and C1 Inhibitor phenotypes.

Author

Ponard D, Gaboriaud C, Charignon D, Ghannam A, Wagenaar-Bos IGA, Roem D, López-Lera A, López-Trascasa M, Tosi M, and Drouet C

Subjects

Alleles, Complement C1 Inhibitor Protein chemistry, Computational Biology, Databases, Genetic, Genotype, Haploinsufficiency, Humans, Models, Molecular, Protein Conformation, RNA Splicing, Structure-Activity Relationship, Angioedemas, Hereditary diagnosis, Angioedemas, Hereditary genetics, Complement C1 Inhibitor Protein genetics, Genetic Association Studies methods, Genetic Predisposition to Disease, Mutation, Phenotype

Abstract

C1 inhibitor (C1Inh) deficiency is responsible for hereditary angioedema (C1-INH-HAE) and caused by variants of the SERPING1/C1INH/C1NH gene. C1Inh is the major control of kallikrein-kinin system. C1Inh deficiency leads to its uncontrolled activation, with subsequent generation of the vasoactive peptide bradykinin. This update documents 748 different SERPING1 variants, including published variants and additional 120 unpublished ones. They were identified as heterozygous variants (n = 729), as homozygous variants in 10 probands and as compound heterozygous variants (nine combinations). Six probands with heterozygous variants exhibited gonadal mosaicism. Probands with heterozygous (n = 72) and homozygous (n = 1) variants were identified as de novo cases. Overall, 58 variants were found at positions showing high residue conservation among serpins, and have been referred to as a mousetrap function of C1Inh: reactive center loop, gate, shutter, breach, and hinge. C1Inh phenotype analysis identified dysfunctional serpin variants with failed serpin-protease association and a residual 105-kDa species after incubation with target protease. Regarding this characteristic, in conditions with low antigenic C1Inh, 74 C1-INH-HAE probands presented with an additional so-called intermediate C1-INH-HAE phenotype. The present update addresses a comprehensive SERPING1 variant spectrum that facilitates genotype-phenotype correlations, highlighting residues of strategic importance for serpin function and for identification of C1Inh deficiency as serpinopathy., (© 2019 Wiley Periodicals, Inc.)

Published

2020

19. Serum complexes between C1INH and C1INH autoantibodies for the diagnosis of acquired angioedema.

Author

López-Lera A, Garrido S, Nozal P, Skatum L, Bygum A, Caballero T, and López Trascasa M

Subjects

Adult, Aged, Aged, 80 and over, Angioedema blood, Angioedema diagnosis, Angioedemas, Hereditary blood, Angioedemas, Hereditary diagnosis, Autoantibodies blood, Autoantibodies metabolism, Cohort Studies, Complement C1 Inhibitor Protein genetics, Complement C1 Inhibitor Protein metabolism, Complement C1q immunology, Complement C1q metabolism, Enzyme-Linked Immunosorbent Assay, Europe, Female, Humans, Male, Middle Aged, Multiprotein Complexes blood, Multiprotein Complexes metabolism, Mutation, Sensitivity and Specificity, Angioedema immunology, Angioedemas, Hereditary immunology, Autoantibodies immunology, Complement C1 Inhibitor Protein immunology, Multiprotein Complexes immunology

Abstract

Acquired angioedema due to C1-inhibitor (C1INH) deficiency (AAE) is caused by secondary C1INH deficiency leading to bradykinin-mediated angioedema episodes. AAE typically presents in adulthood and is associated with B cell lymphoproliferation. Anti-C1INH autoantibodies (antiC1INHAbs) are detectable in a subset of AAE cases and considered a hallmark of the disease. When free antiC1INHAbs and malignant tumors are not detectable, diagnosis relies on the finding of low C1INH levels and/or function, lack of family history and SERPING1 mutations, age at onset and low or undetectable C1q levels, none of which is specific for AAE. We tested the diagnostic value of a novel enzyme-linked immunosorbent assay (ELISA) for the detection of circulating complexes between C1INH and antiC1INHAbs (C1INH-antiC1INHAb) in the serum of 20 European AAE patients characterized on the basis of their complement levels and function. Free antiC1INHAbs were detected in nine of 20 patients [six of immunoglobulin (Ig)G class, two of IgM class and one simultaneously presenting IgG and IgM classes], whereas C1INH-antiC1INHAb complexes were found in 18 of 20 of the AAE cases, regardless of the presence or absence of detectable free anti-C1INHAbs. Of note, nine of 20 patients showed negative free antiC1INHabs, but positive C1INH-antiC1INHAb complexes in their first measurement. In the cohort presented, IgM-class C1INH-antiC1INHAb are specifically and strongly associated with low C1q serum levels. Detection of C1INH-antiC1-INHAbs provides an added value for AAE diagnosis, especially in those cases in whom no free anti-C1INH antibodies are detected. The link between IgM-class C1INH-antiC1INHAb complexes and C1q consumption could have further implications for the development of autoimmune manifestations in AAE., (© 2019 British Society for Immunology.)

Published

2019

20. Hereditary Angioedema: Insights into inflammation and allergy.

Author

Maas C and López-Lera A

Subjects

Blood Coagulation immunology, Bradykinin immunology, Complement System Proteins immunology, Fibrinolysis immunology, Humans, Hypersensitivity immunology, Hypersensitivity pathology, Phenotype, Angioedemas, Hereditary immunology, Angioedemas, Hereditary pathology, Inflammation immunology, Inflammation pathology

Abstract

Hereditary Angioedema (HAE) is a rare autosomal recessive bradykinin (BK)-mediated disease characterized by local episodes of non-pitting swelling. Initially considered a complement-mediated disease, novel pathogenic mechanisms uncovered in the last decade have revealed new HAE-associated genes and tight physiological relationships among complement, contact, coagulation, fibrinolysis and inflammation. Uncontrolled production of BK due to inefficient regulation of the plasma contact system, increased activity of contact and coagulation factors or a deficient regulation of BK receptor-triggered intracellular signalling are on the basis of HAE pathology. In this new scenario, HAE can result from different mechanisms that may generate distinct clinical phenotypes of the disease. This review focuses in the recent advances and unsolved challenges in our comprehension of this ever increasingly complex pathology., (Copyright © 2019 Elsevier Ltd. All rights reserved.)

Published

2019

21. Complement as a diagnostic tool in immunopathology.

Author

López-Lera A, Corvillo F, Nozal P, Regueiro JR, Sánchez-Corral P, and López-Trascasa M

Subjects

Autoimmune Diseases immunology, Complement System Proteins metabolism, Humans, Immune Tolerance, Immunity, Innate, Autoimmune Diseases diagnosis, Communicable Diseases diagnosis, Communicable Diseases immunology, Complement System Proteins immunology, Neurodegenerative Diseases diagnosis, Neurodegenerative Diseases immunology, Sepsis diagnosis, Sepsis immunology

Abstract

The complement system is a complex and autoregulated multistep cascade at the interface of innate and adaptive immunity. It is activated by immune complexes or apoptotic cells (classical pathway), pathogen-associated glycoproteins (lectin pathway) or a variety of molecular and cellular surfaces (alternative pathway). Upon activation, complement triggers the generation of proteolytic fragments that allow the elimination of the activating surface by enhancing inflammation, opsonization, phagocytosis, and cellular lysis. Moreover, complement efficiently discriminates self from non-self surfaces by means of soluble and membrane-bound complement regulators which are critical for innate self-tolerance. Complement deficiency or dysfunction disturb complement homeostasis and give rise to diseases as diverse as bacterial infections, autoimmunity, or renal and neurological disorders. Research on complement-targeted therapies is an expanding field that has already improved the prognosis of severe diseases such as atypical Haemolytic Uremic syndrome or Paroxysmal Nocturnal Haemoglobinuria. Therefore, complement analysis and monitoring provides valuable information with deep implications for diagnosis and therapy. In addition to its important role as an extracellular defense system, it has now become evident that complement is also present intracellularly, and its activation has profound implications for leukocyte survival and function. In this review, we summarize the essential, up-to-date information on the use of complement as a diagnostic and therapeutic tool in the clinics., (Copyright © 2018 Elsevier Ltd. All rights reserved.)

Published

2019

22. Common and rare genetic variants of complement components in human disease.

Author

Goicoechea de Jorge E, López Lera A, Bayarri-Olmos R, Yebenes H, Lopez-Trascasa M, and Rodríguez de Córdoba S

Subjects

Humans, Complement System Proteins genetics, Genetic Predisposition to Disease genetics, Genetic Variation genetics

Abstract

Genetic variability in the complement system and its association with disease has been known for more than 50 years, but only during the last decade have we begun to understand how this complement genetic variability contributes to the development of diseases. A number of reports have described important genotype-phenotype correlations that associate particular diseases with genetic variants altering specific aspects of the activation and regulation of the complement system. The detailed functional characterization of some of these genetic variants provided key insights into the pathogenic mechanisms underlying these pathologies, which is facilitating the design of specific anti-complement therapies. Importantly, these analyses have sometimes revealed unknown features of the complement proteins. As a whole, these advances have delineated the functional implications of genetic variability in the complement system, which supports the implementation of a precision medicine approach based on the complement genetic makeup of the patients. Here we provide an overview of rare complement variants and common polymorphisms associated with disease and discuss what we have learned from them., (Copyright © 2018 Elsevier Ltd. All rights reserved.)

Published

2018

23. Autoantibodies Against Perilipin 1 as a Cause of Acquired Generalized Lipodystrophy.

Author

Corvillo F, Aparicio V, López-Lera A, Garrido S, Araújo-Vilar D, de Miguel MP, and López-Trascasa M

Subjects

3T3-L1 Cells, Adipocytes cytology, Adolescent, Adult, Animals, Autoantibodies blood, Biomarkers blood, Cells, Cultured, Child, Female, Humans, Lipid Droplets immunology, Lipid Droplets metabolism, Lipodystrophy, Congenital Generalized blood, Lipodystrophy, Congenital Generalized diagnosis, Lipolysis immunology, Male, Mice, Middle Aged, Perilipin-1 metabolism, Adipocytes immunology, Autoantibodies immunology, Lipodystrophy, Congenital Generalized immunology, Perilipin-1 immunology

Abstract

Acquired generalized lipodystrophy (AGL) is a rare condition characterized by an altered distribution of adipose tissue and predisposition to develop hepatic steatosis and fibrosis, diabetes, and hypertriglyceridemia. Diagnosis of AGL is based on the observation of generalized fat loss, autoimmunity and lack of family history of lipodystrophy. The pathogenic mechanism of fat destruction remains unknown but evidences suggest an autoimmune origin. Anti-adipocyte antibodies have been previously reported in patients with AGL, although their involvement in the pathogenesis has been poorly studied and the autoantibody target/s remain/s to be identified. Using a combination of immunochemical and cellular studies, we investigated the presence of anti-adipocyte autoantibodies in patients with AGL, acquired partial lipodystrophy, localized lipoatrophy due to intradermic insulin injections or systemic lupus erythematosus. Moreover, the impact of anti-adipocyte autoantibodies from AGL patients was assessed in cultured mouse preadipocytes. Following this approach, we identified anti-perilipin 1 IgG autoantibodies in the serum of patients with autoimmune variety-AGL, but in no other lipodystrophies tested. These autoantibodies altered the ability of perilipin 1 to regulate lipolysis in cultured preadipocytes causing abnormal, significantly elevated basal lipolysis. Our data provide strong support for the conclusion that perilipin 1 autoantibodies are a cause of generalized lipodystrophy in these patients.

Published

2018

24. Targeted next-generation sequencing for the molecular diagnosis of hereditary angioedema due to C1-inhibitor deficiency.

Author

Loules G, Zamanakou M, Parsopoulou F, Vatsiou S, Psarros F, Csuka D, Porebski G, Obtulowicz K, Valerieva A, Staevska M, López-Lera A, López-Trascasa M, Moldovan D, Magerl M, Maurer M, Speletas M, Farkas H, and Germenis AE

Subjects

Angioedemas, Hereditary genetics, Case-Control Studies, Chromosomes, Human, Pair 11 genetics, DNA Copy Number Variations, Female, Humans, Male, Polymorphism, Single Nucleotide, Sensitivity and Specificity, Angioedemas, Hereditary diagnosis, Complement C1 Inhibitor Protein genetics, High-Throughput Nucleotide Sequencing methods, Molecular Diagnostic Techniques methods, Sequence Analysis, DNA methods

Abstract

SERPING1 genotyping of subjects suspicious for hereditary angioedema due to C1-INH deficiency (C1-INH-HAE) is important for clinical practice as well as for research reasons. Conventional approaches towards the detection of C1-INH-HAE-associated SERPING1 variants are cumbersome and time-demanding with many pitfalls. To take advantage of the benefits of next-generation sequencing (NGS) technology, we developed and validated a custom NGS platform that, by targeting the entire SERPING1 gene, facilitates genetic testing of C1-INH-HAE patients in clinical practice. In total, 135 different C1-INH-HAE-associated SERPING1 variants, out of the approximately 450 reported, along with 115 negative controls and 95 randomly selected DNA samples from affected family members of C1-INH-HAE index patients, were included in the forward and reverse validation processes of this platform. Our platform's performance, i.e. analytical sensitivity of 98.96%, a false negative rate of 1.05%, analytical specificity 100%, a false positive rate equal to zero, accuracy of 99.35%, and repeatability of 100% recommends its implementation as a first line approach for the genetic testing of C1-INH-HAE patients or as a confirmatory method. A noteworthy advantage of our platform is the concomitant detection of single nucleotide variants and copy number variations throughout the whole length of the SERPING1 gene, moreover providing information about the size and the localization of the latter. During our study, 15 novel C1-INH-HAE-related SERPING1 variants were detected., (Copyright © 2018 Elsevier B.V. All rights reserved.)

Published

2018

25. High Complement Factor H-Related (FHR)-3 Levels Are Associated With the Atypical Hemolytic-Uremic Syndrome-Risk Allele CFHR3*B .

Author

Pouw RB, Gómez Delgado I, López Lera A, Rodríguez de Córdoba S, Wouters D, Kuijpers TW, and Sánchez-Corral P

Subjects

Adolescent, Adult, Alleles, Atypical Hemolytic Uremic Syndrome blood, Child, Child, Preschool, Complement Factor H analysis, Complement Pathway, Alternative, Enzyme-Linked Immunosorbent Assay, Haplotypes, Humans, Infant, Infant, Newborn, Young Adult, Atypical Hemolytic Uremic Syndrome genetics, Blood Proteins genetics, Genetic Predisposition to Disease

Abstract

Dysregulation of the complement alternative pathway (AP) is a major pathogenic mechanism in atypical hemolytic-uremic syndrome (aHUS). Genetic or acquired defects in factor H (FH), the main AP regulator, are major aHUS drivers that associate with a poor prognosis. FH activity has been suggested to be downregulated by homologous FH-related (FHR) proteins, including FHR-3 and FHR-1. Hence, their relative levels in plasma could be disease-relevant. The genes coding for FH, FHR-3, and FHR-1 ( CFH, CFHR3 , and CFHR1 , respectively) are polymorphic and located adjacent to each other on human chromosome 1q31.3. We have previously shown that haplotype CFH(H3)-CFHR3*B-CFHR1*B associates with aHUS and reduced FH levels. In this study, we used a specific enzyme-linked immunosorbent assay to quantify FHR-3 in plasma samples from controls and patients with aHUS genotyped for the three known CFHR3 alleles ( CFHR3*A, CFHR3*B , and CFHR3*Del ). In the 218 patients carrying at least one copy of CFHR3 , significant differences between CFHR3 genotype groups were found, with CFHR3*A/Del patients having the lowest FHR-3 concentration (0.684-1.032 µg/mL), CFHR3*B/Del and CFHR3*A/A patients presenting intermediate levels (1.437-2.201 µg/mL), and CFHR3*A/B and CFHR3*B/B patients showing the highest concentration (2.330-4.056 µg/mL) ( p  < 0.001). These data indicate that CFHR3*A is a low-expression allele, whereas CFHR3*B , associated with increased risk of aHUS, is a high-expression allele. Our study reveals that the aHUS-risk haplotype CFH(H3)-CFHR3*B-CFHR1*B generates twofold more FHR-3 than the non-risk CFH(H1)-CFHR3*A-CFHR1*A haplotype. In addition, FHR-3 levels were higher in patients with aHUS than in control individuals with the same CFHR3 genotype. These data suggest that increased plasma levels of FHR-3, altering the balance between FH and FHR-3, likely impact the FH regulatory functions and contribute to the development of aHUS.

Published

2018

26. Human plasma C3 is essential for the development of memory B, but not T, lymphocytes.

Author

Jiménez-Reinoso A, Marin AV, Subias M, López-Lera A, Román-Ortiz E, Payne K, Ma CS, Arbore G, Kolev M, Freeley SJ, Kemper C, Tangye SG, Fernández-Malavé E, Rodríguez de Córdoba S, López-Trascasa M, and Regueiro JR

Subjects

B-Lymphocytes immunology, B-Lymphocytes pathology, Complement C3 immunology, Female, Humans, Male, T-Lymphocytes, Helper-Inducer immunology, T-Lymphocytes, Helper-Inducer pathology, B-Lymphocytes metabolism, Complement C3 metabolism, Immunologic Memory, T-Lymphocytes, Helper-Inducer metabolism

Published

2018

27. Complement Study Versus CINH Gene Testing for the Diagnosis of Type I Hereditary Angioedema in Children.

Author

Pedrosa M, Phillips-Angles E, López-Lera A, López-Trascasa M, and Caballero T

Subjects

Adolescent, Bradykinin metabolism, Child, Child, Preschool, Complement Activation genetics, Complement C1 Inactivator Proteins genetics, Complement C1 Inhibitor Protein, DNA Mutational Analysis, Early Diagnosis, Female, Humans, Infant, Male, Mutation genetics, Pedigree, Complement C1 Inactivator Proteins metabolism, Hereditary Angioedema Types I and II diagnosis

Published

2016

28. C1 inhibitor function using contact-phase proteases as target: evaluation of an innovative assay.

Author

Ghannam A, Sellier P, Defendi F, Favier B, Charignon D, López-Lera A, López-Trascasa M, Ponard D, and Drouet C

Subjects

Angioedemas, Hereditary diagnosis, Angioedemas, Hereditary immunology, Angioedemas, Hereditary metabolism, Biological Assay methods, Biological Assay standards, Estrogens metabolism, Factor XIIa metabolism, Female, Humans, Kininogens metabolism, Male, Prekallikrein metabolism, Protein Binding, ROC Curve, Reference Values, Reproducibility of Results, alpha-Macroglobulins metabolism, Complement C1 Inactivator Proteins metabolism, Peptide Hydrolases metabolism

Abstract

Background: Controlling prekallikrein activation by C1 inhibitor (C1Inh) represents the most essential mechanism for angioedema patient protection. C1Inh function in the plasma is usually measured based on the residual activity of the C1s protease not involved in the pathological process. We have hereby proposed an alternative enzymatic measurement of C1Inh function based on contact-phase activation and correlation with angioedema diagnostic requirements., Methods: The contact phase was reconstituted using the purified components, with C1Inh standard or plasma sample. The kinetics of the amidase activity were monitored using Pro-Phe-Arg-pNA, independently of alpha2-macroglobulin. We prevented any interference from a possible high plasma kininogenase activity by preincubating the samples with protease inhibitor. Receiver operating characteristics (ROC) were used to calculate the assay's diagnostic performance., Results: The calibration curve was built using C1Inh standard (threshold limit 0.10 × 10(-3) U, i.e., 0.2 pmol), and C1Inh function was quantified in the sample, with a reference interval established based on healthy individuals (n = 281; men: 0.61-1.10 U/ml, median: 0.85 U/ml; women: 0.42-1.08 U/ml, median: 0.74 U/ml). The median values of female donors were lower than those of the others due to estrogen, yet C1Inh function remained within the reference interval. The ROC curve calculation provided the following optimum diagnostic cutoff values: women 0.36 U/ml (area under curve [AUC]: 0.99; sensitivity: 93.48%; specificity: 99.37%); and men 0.61 U/ml (AUC: 1; sensitivity: 100.0%; specificity: 100.0%)., Conclusion: The performance outcome provided features suitable for angioedema diagnostic or follow-up. Established by means of the kinin formation process, this assay should be preferred over the method based on a C1s protease target., (© 2015 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2015

29. Similar percentages in most abundant chronic granulomatous disease autosomal recessive forms in a Spanish cohort.

Author

Pérez de Diego R, López-Lera A, and Ferreira A

Subjects

Cohort Studies, Humans, NADPH Oxidases deficiency, Spain, White People genetics, Granulomatous Disease, Chronic genetics, NADPH Oxidases genetics

Published

2015

30. Expression of the SERPING1 gene is not regulated by promoter hypermethylation in peripheral blood mononuclear cells from patients with hereditary angioedema due to C1-inhibitor deficiency.

Author

López-Lera A, Pernia O, López-Trascasa M, and Ibanez de Caceres I

Subjects

Angioedemas, Hereditary blood, Complement C1 Inactivator Proteins metabolism, Complement C1 Inhibitor Protein, CpG Islands, Humans, RNA, Messenger genetics, Angioedemas, Hereditary genetics, Complement C1 Inactivator Proteins genetics, DNA Methylation, Monocytes metabolism, Promoter Regions, Genetic

Abstract

SERPING1 mutations causing Hereditary Angioedema type I (HAE-I) due to C1-Inhibitor (C1-INH) deficiency display a dominant-negative effect usually resulting in protein levels far below the expected 50%. To further investigate mechanisms for its reduced expression, we analyzed the promoter DNA methylation status of SERPING1 and its influence on C1-INH expression. Global epigenetic reactivation correlated with C1-INH mRNA synthesis and protein secretion in Huh7 hepatoma cells. However, PBMCs extracted from controls, HAE-I and HAE-II patients presented identical methylation status of the SERPING1 promoter when analyzed by bisulphite sequencing; the proximal CpG island (exon 2) is constitutively unmethylated, while the most distant one (5.7Kb upstream the transcriptional start site) is fully methylated. These results correlate with the methylation profile observed in Huh7 cells and indicate that there is not a direct epigenetic regulation of C1-INH expression in PBMCs specific for each HAE type. Other indirect modes of epigenetic regulation cannot be excluded.

Published

2014

31. Rothmund-Thomson syndrome and glomerulonephritis in a homozygous C1q-deficient patient due to a Gly164Ser C1qC mutation.

Author

López-Lera A, Torres-Canizales JM, Garrido S, Morales A, and López-Trascasa M

Subjects

Adult, Cataract complications, Cataract genetics, Cohort Studies, Erythema complications, Erythema genetics, Exons, Glomerulonephritis complications, Glycine chemistry, Homozygote, Humans, Introns, Male, Mutation, Phenotype, Rothmund-Thomson Syndrome complications, Serine chemistry, Skin Diseases complications, Skin Diseases genetics, Spain, Complement C1q genetics, Glomerulonephritis diagnosis, Glomerulonephritis genetics, Rothmund-Thomson Syndrome diagnosis, Rothmund-Thomson Syndrome genetics

Published

2014

32. Hereditary angioedema caused by the p.Thr309Lys mutation in the F12 gene: a multifactorial disease.

Author

Gómez-Traseira C, López-Lera A, Drouet C, López-Trascasa M, Pérez-Fernández E, Favier B, Prior N, and Caballero T

Subjects

Adolescent, Adult, Factor XII chemistry, Family, Female, Humans, Lysine genetics, Male, Pedigree, Severity of Illness Index, Spain, Threonine genetics, Young Adult, Angioedemas, Hereditary genetics, Angioedemas, Hereditary physiopathology, Factor XII genetics, Hereditary Angioedema Type III genetics, Mutation

Published

2013

33. Disease-modifying factors in hereditary angioedema: an RNA expression-based screening.

Author

López-Lera A, Cabo FS, Garrido S, Dopazo A, and López-Trascasa M

Subjects

Complement C1 Inhibitor Protein genetics, Family, Female, Gene Expression Regulation, Hereditary Angioedema Types I and II metabolism, Humans, Male, Middle Aged, Oligonucleotide Array Sequence Analysis, Pedigree, RNA genetics, Reverse Transcriptase Polymerase Chain Reaction, Complement C1 Inhibitor Protein metabolism, Genetic Association Studies, Hereditary Angioedema Types I and II genetics, Hereditary Angioedema Types I and II physiopathology, Leukocytes, Mononuclear metabolism, Mutation, RNA metabolism

Abstract

Background: Hereditary Angioedema due to C1-Inhibitor deficiency (HAE types I and II) is a monogenic disease characterized by sudden, self-limited episodes of cutaneous and mucosal swelling due to local deregulation of vascular permeability. Despite its monogenic pattern of inheritance, HAE exhibits great clinical variability and low genotype/phenotype correlation among those affected, which ultimately hinders therapeutic approach and probably underlies yet unknown genetic and environmental factors., Methods: We studied whole-genome RNA expression of PBMCs in three HAE type-I families (accounting for 40 individuals), 24 of which carry the same R472X mutation in the C1-Inhibitor gene and show large variability in terms of disease expression. Those included in this study were analyzed according to the presence of mutation and/or clinical symptoms., Results: Instead of a single, common disease-associated expression pattern, we found different transcriptome signatures in two of the families studied. In one of them (referred to as DR family), symptoms correlate with the upregulation of 35 genes associated to the biological response to viral infections (including RSADs, OAS, MX and ISG pathway members) and immune response. In another pedigree (Q family), disease manifestation is linked to the upregulation of 43 genes with diverse functions, including transcription and protein folding. Moreover, symptoms-free members of the Q pedigree display relatively higher expression of 394 genes with a wide diversity of functions., Conclusion: We found no evidence for a common altered PBMC expression pattern linked to HAE symptoms in the three families analyzed. All the data considered, differential gene expression in PBMCs do not seem to play a significant role in the predisposition or protection against HAE in the basal -between crises- conditions analyzed. Although the RNA expression pattern associated to the response to viral infections observed in the DR family supports the idea of infectious diseases as a modifying factor for HAE severity, large-scale studies would be needed to statistically associate such expression pattern to the development of this rare disease.

Published

2013

34. High frequency in the delay in primary tooth loss in X-linked chronic granulomatous disease.

Author

Pérez de Diego R, López Lera A, and Cerdán AF

Subjects

Adolescent, Child, Europe epidemiology, Granulomatous Disease, Chronic epidemiology, Granulomatous Disease, Chronic pathology, Humans, Membrane Glycoproteins metabolism, Mutation, NADPH Oxidase 2, NADPH Oxidases metabolism, Time Factors, Tooth, Deciduous pathology, Granulomatous Disease, Chronic genetics, Membrane Glycoproteins genetics, NADPH Oxidases genetics, Tooth, Deciduous enzymology

Published

2012

35. Clinical, biochemical, and genetic characterization of type III hereditary angioedema in 13 Northwest Spanish families.

Author

Marcos C, López Lera A, Varela S, Liñares T, Alvarez-Eire MG, and López-Trascasa M

Subjects

Adult, Aged, Complement C1 Inhibitor Protein genetics, Complement C1 Inhibitor Protein metabolism, Factor XII metabolism, Family, Female, Humans, Male, Middle Aged, Mutation, Pregnancy, Pregnancy Complications epidemiology, Pregnancy Complications genetics, Pregnancy Complications metabolism, Spain epidemiology, Young Adult, Factor XII genetics, Hereditary Angioedema Type III epidemiology, Hereditary Angioedema Type III genetics, Hereditary Angioedema Type III metabolism, Hereditary Angioedema Type III physiopathology

Abstract

Background: A new variant of hereditary angioedema has been reported during the last decade. Three main characteristics distinguish it from classic hereditary angioedema: normal C1 inhibitor activity, predominance in women, and different genetic alterations., Objective: To assess the symptoms, laboratory findings, and treatment of a population with type III hereditary angioedema from Northwest Spain., Methods: We studied 29 patients (26 female and 3 male) from 13 different families., Results: The 26 female patients showed a similar clinical pattern to the classic forms of hereditary angioedema, and 22 of these patients had the estrogen-dependent phenotype. Three patients had a negative family history, and 1 of the parents was confirmed as an asymptomatic carrier in 2 of them. All had functional C1 inhibitor activity within the normal range in periods without high estrogen levels, but during attacks (in female patients) and pregnancy, activity decreased to below 50%. One male patient had normal C1 inhibitor activity during attacks, and he was initially diagnosed as having idiopathic angioedema. The C4 and antigenic C1 inhibitor levels were always normal. All studied patients had the c.1032C>A, Thr309Lys mutation in the factor XII gene. The mutation was also found in asymptomatic relatives: 5 of 6 men studied and 1 of 8 women studied., Conclusion: Positive family history is a diagnosis criterion, but it could be lacking because there may be asymptomatic relatives, primarily males., (Copyright © 2012 American College of Allergy, Asthma & Immunology. Published by Elsevier Inc. All rights reserved.)

Published

2012

36. Complement factor I deficiency: a not so rare immune defect: characterization of new mutations and the first large gene deletion.

Author

Alba-Domínguez M, López-Lera A, Garrido S, Nozal P, González-Granado I, Melero J, Soler-Palacín P, Cámara C, and López-Trascasa M

Subjects

Adult, Bacterial Infections immunology, Child, Child, Preschool, Complement C3 deficiency, Complement C3 genetics, Complement C3 immunology, Complement C3 metabolism, Complement C4 metabolism, Complement Factor I deficiency, Exons, Family, Female, Genetic Diseases, Inborn genetics, Genetic Diseases, Inborn immunology, Hereditary Complement Deficiency Diseases, Heterozygote, Homozygote, Humans, Male, Pedigree, Recurrence, Spain, Bacterial Infections complications, Complement Factor I genetics, Gene Deletion, Genetic Diseases, Inborn complications, Genetic Diseases, Inborn diagnosis, Mutation

Abstract

Background: Complement Factor I (CFI) is a serine protease with an important role in complement alternative pathway regulation. Complete factor I deficiency is strongly associated with severe infections. Approximately 30 families with this deficiency have been described worldwide., Patients and Methods: We have studied five new Spanish families suffering from CFI deficiency. From 19 screened people, 7 homozygous, 10 heterozygous and 2 healthy subjects were identified. Clinical, biochemical and genetic descriptions are included., Results: Molecular studies demonstrated 4 novel mutations in the screened individuals; amongst them, we describe here the first great gene deletion reported in the CFI locus, which includes full exon 2 and part of the large intron 1., Conclusion: CFI deficiency is possibly an underestimated defect and the eventual existence of this deficiency should be tested in those patients exhibiting low C3 and recurrent bacterial infections. We propose a simple diagnostic flowchart to help clinicians in the identification and correct diagnosis of such patients.

Published

2012

37. Analysis of SERPING1 expression on hereditary angioedema patients: quantitative analysis of full-length and exon 3 splicing variants.

Author

de la Cruz RM, López-Lera A, and López-Trascasa M

Subjects

Adolescent, Adult, Angioedemas, Hereditary classification, Angioedemas, Hereditary epidemiology, Complement C1 Inhibitor Protein, DNA Mutational Analysis, Exons genetics, Female, Gene Expression Regulation, Gene Frequency, Genetic Association Studies, Genetic Loci, Humans, Male, Middle Aged, Spain, Alternative Splicing, Angioedemas, Hereditary genetics, Complement C1 Inactivator Proteins genetics, Mutation genetics, Protein Isoforms genetics

Abstract

Hereditary angioedema (HAE) due to C1-inhibitor (C1-Inh) deficiency is an autosomal dominant disease caused by mutations in the SERPING1 locus. According to protein levels in plasma, two HAE phenotypes have been described: Type I, with low circulating protein levels in plasma, and Type II, where the protein is present but dysfunctional. Although more than 200 mutations have been described to date, studies on the molecular basis of this autosomic dominant trait are scarce. Previous studies demonstrated that C1-Inh mRNA expression was decreased in HAE patients. Herein, we have confirmed these findings in a large series of Spanish patients. Moreover, when our data were analyzed taking into account the type of mutation carried by the patient (i.e., missense, frameshift,…), significant differences were amongst the control, nonsense and splicing mutations groups (P<0.05). By opposite, no differences in C1-Inh mRNA expression were found between the control and HAE Type II groups, nor between treated and untreated patients groups, although a significant difference was observed between controls and untreated HAE Type I patients. An alternative splicing event has been described in the SERPING1 locus resulting in two different transcripts: the full-length and a shorter variant with skipping of exon 3. In order to investigate a possible role for this splicing in HAE, we quantified both mRNA variants in a series of 28 patients. No statistical differences were found in the expression of both variants between controls and patients when compared. However, a separate analysis considering each type of mutation evidenced a significant decrease (P: 0.0156) in the expression of the exon 3 skipping variant in those HAE Type I patients carrying nonsense mutations. Besides, median of the full variant's copy number was statistically decreased on the splicing group when compared with either stop and/or missense groups. The results of these studies provide new data about C1 inhibitor expression in HAE patients and shed more light on the transcriptional regulation of the SERPING1 locus. Quantitative analysis of splicing variants could help to determine the eventual variations of these two transcripts and their possible role under inflammatory stimuli., (Copyright © 2011 Elsevier B.V. All rights reserved.)

Published

2012

38. SERPING1 mutations in 59 families with hereditary angioedema.

Author

López-Lera A, Garrido S, Roche O, and López-Trascasa M

Subjects

Angioedemas, Hereditary blood, Cohort Studies, Complement C1 Inactivator Proteins analysis, Complement C1 Inhibitor Protein, Complement C3 analysis, Complement C4 analysis, DNA Mutational Analysis, Female, Humans, Male, Angioedemas, Hereditary genetics, Complement C1 Inactivator Proteins genetics, Mutation

Abstract

Hereditary angioedema due to C1 Inhibitor (C1Inh) deficiency (HAE types I and II) is a rare, life-threatening disease causing spontaneous edema of the submucosal layers. A cohort of 127 individuals with symptoms of recurrent familial angioedema from 59 non-related families was studied. All the patients included fulfilled the diagnostic and biochemical criteria of HAE, including low C1Inh function and/or concentration. Genetic studies were carried out by PCR and sequencing of the C1NH locus followed, in the negative cases, by MLPA, long-range PCR and restriction enzyme analysis of genomic DNA to detect potential large rearrangements. Mutations located in consensus splicing sequences or nearby positions were studied by RT-PCR. The study identified 52 different mutations (25 missense, 15 frameshift, 7 splicing defects and 5 large deletions) responsible for the disease in 56 HAE families. In the remaining three families no molecular alteration could be detected. Twenty-seven of the mutations in this cohort are novel and 10 are confirmed de novo cases. The pathologic effect of the 5 splicing defects first reported here was assessed at the RNA and protein levels. Large deletions affecting exons 4 and 7, ranging from approximately 1500 to 2500 bp, were partially characterized by their altered restriction patterns upon long-range amplification. These results highlight the heterogeneity of mutations in the C1NH gene causing C1Inh deficiency and HAE. An approach to the molecular effects associated to each of the mutations reported here was made when possible based on the available data of pathological variants of serpins., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2011

39. A new case of homozygous C1-inhibitor deficiency suggests a role for Arg378 in the control of kinin pathway activation.

Author

López-Lera A, Favier B, de la Cruz RM, Garrido S, Drouet C, and López-Trascasa M

Subjects

Adult, Angioedemas, Hereditary diagnosis, Angioedemas, Hereditary metabolism, Cell Line, Transformed, Child, Preschool, Complement C1 Inhibitor Protein genetics, DNA Mutational Analysis, Disease Progression, Family, Female, Homozygote, Humans, Male, Mutant Proteins genetics, Mutation genetics, Nephelometry and Turbidimetry, Plasma Kallikrein metabolism, Protein Binding genetics, Protein Binding immunology, Protein Conformation, Transgenes genetics, Angioedemas, Hereditary genetics, Angioedemas, Hereditary physiopathology, Complement C1 Inhibitor Protein metabolism, Complement C1q deficiency, Mutant Proteins metabolism

Published

2010

40. Molecular characterization of three new mutations causing C5 deficiency in two non-related families.

Author

López-Lera A, Garrido S, de la Cruz RM, Fontán G, and López-Trascasa M

Subjects

Complement C5 immunology, Female, Heterozygote, Humans, Male, Meningitis, Meningococcal immunology, Models, Molecular, Mutation, Neisseria meningitidis, Serogroup B, Complement C5 genetics, Meningitis, Meningococcal genetics

Abstract

Deficiencies in complement components are rare diseases whose diagnosis is often underestimated. In addition, in only a few cases molecular studies have been carried out for the characterization of the underlying genetic defects. To date, studies involving C5-deficient patients are scarce. The aim of the present report is to characterize the biochemical and molecular complement deficiency in two non-related families with one or more members showing no detectable hemolytic complement activity (CH50<50 U/ml) and reporting a history of several episodes of meningitis. Protein deficiency was assessed by means of hemolytic assays, bi-dimensional double immunodiffusion, ELISA and Western blot of patients' sera. Molecular studies were carried out by PCR and RT-PCR of DNA and RNA, respectively, both extracted from fresh blood samples of each family member. In Family A, only the propositus had complete C5 deficiency. Molecular studies showed that he was heterozygous for two changes in the C5 gene. One of the mutations was also carried by the father (c.1883&#95;1884AGC, Y846H) was a de novo mutation. In Family B, the two C5-deficient members share the homozygous nonsense mutation c.892C>T (Q298X) in exon 9. The characterization of these new mutations is interesting in order to elucidate structure-function relationships in the C5 gene and it also helps to understand the molecular basis of this uncommon deficiency. Moreover, this report highlights the importance of complement screening in cases of repeated meningococcal infections in order to establish its involvement and to consider adequate clinical recommendations such as prophylactic antibiotics or meningococcal vaccines.

Published

2009