Your search keyword '"Corveleyn, Anniek"' showing total 23 results

1. Child Neurology: Familial Hemophagocytic Lymphohistiocytosis Underlying Isolated Central Nervous System Inflammation.

Author

Bucciol, Giorgia, Willemyns, Nele, Verhaaren, Benjamin, Bossuyt, Xavier, Lagrou, Katrien, Corveleyn, Anniek, Moshous, Despina, Jansen, Katrien, De Waele, Liesbeth, and Meyts, Isabelle

Published

2022

2. A Novel Kindred with MyD88 Deficiency.

Author

Bucciol, Giorgia, Moens, Leen, Corveleyn, Anniek, Dreesman, Alexandra, and Meyts, Isabelle

Subjects

CHICKENPOX, MYELOID differentiation factor 88, MONONUCLEAR leukocytes

Abstract

The patient was in good clinical condition and did not experience recurrent infections after the start of Ig replacement therapy and antibiotic prophylaxis with amoxicillin until the age of 5 years, when he was admitted to a hospital with COVID-19 pneumonia requiring oxygen therapy for 4 days. Invasive infections with viruses, mycobacteria, parasites, and fungi have not been described in human MyD88 deficiency, although one patient had Bacillus Calmette-Guérin (BCG) adenitis after vaccination with BCG [[2], [5]]. We here present a patient carrying a homozygous deleterious mutation in I MYD88 i , who experienced viral infections and recurrent mucocutaneous candidiasis in addition to the classical invasive and superficial pyogenic infections. [Extracted from the article]

Published

2022

3. Clinical characterization of the first Belgian SCN5A founder mutation cohort.

Author

Sieliwonczyk, Ewa, Alaerts, Maaike, Robyns, Tomas, Schepers, Dorien, Claes, Charlotte, Corveleyn, Anniek, Willems, Rik, Craenenbroeck, Emeline M Van, Simons, Eline, Nijak, Aleksandra, Vandendriessche, Bert, Mortier, Geert, Vrints, Christiaan, Koopman, Pieter, Heidbuchel, Hein, Laer, Lut Van, Saenen, Johan, Loeys, Bart, Van Craenenbroeck, Emeline M, and Van Laer, Lut

Subjects

GENETIC mutation, BRUGADA syndrome, MEMBRANE transport proteins, ELECTROCARDIOGRAPHY, PHENOTYPES

Abstract

Aims: We identified the first Belgian SCN5A founder mutation, c.4813 + 3_4813 + 6dupGGGT. To describe the clinical spectrum and disease severity associated with this mutation, clinical data of 101 SCN5A founder mutation carriers and 46 non-mutation carrying family members from 25 Belgian families were collected.Methods and Results: The SCN5A founder mutation was confirmed by haplotype analysis. The clinical history and electrocardiographic parameters of the mutation carriers and their family members were gathered and compared. A cardiac electrical abnormality was observed in the majority (82%) of the mutation carriers. Cardiac conduction defects, defined as PR or QRS prolongation on electrocardiogram (ECG), were most frequent, occurring in 65% of the mutation carriers. Brugada syndrome (BrS) was the second most prevalent phenotype identified in 52%, followed by atrial dysrythmia in 11%. Overall, 33% of tested mutation carriers had a normal sodium channel blocker test. Negative tests were more common in family members distantly related to the proband. Overall, 23% of the mutation carriers were symptomatic, with 8% displaying major adverse events. As many as 13% of the patients tested with a sodium blocker developed ventricular arrhythmia. One family member who did not carry the founder mutation was diagnosed with BrS.Conclusion: The high prevalence of symptoms and sensitivity to sodium channel blockers in our founder population highlights the adverse effect of the founder mutation on cardiac conduction. The large phenotypical heterogeneity, variable penetrance, and even non-segregation suggest that other genetic (and environmental) factors modify the disease expression, severity, and outcome in these families. [ABSTRACT FROM AUTHOR]

Published

2021

4. Whole exome sequencing in a large pedigree with DCM identifies a novel mutation in RBM20.

Author

Robyns, Tomas, Willems, Rik, Van Cleemput, Johan, Jhangiani, Shalini, Muzny, Donna, Gibbs, Richard, Lupski, James R., Breckpot, Jeroen, Devriendt, Koenraad, and Corveleyn, Anniek

Subjects

DILATED cardiomyopathy, TREATMENT of cardiomyopathies, ARRHYTHMIA, HEART disease diagnosis, HEART failure treatment

Abstract

Background: Familial dilated cardiomyopathy (DCM) is genetically heterogeneous and is associated with mutations in at least 40 different genes. Apart from TTN encoding the giant protein Titin, none of these genes have an expected diagnostic yield of more than 5% complicating genetic diagnosis. Whole exome sequencing (WES) is a powerful alternative for the identification of the causal gene, however variant interpretation remains challenging. We report on WES in a large family with autosomal dominant DCM complicated by end stage heart failure and non-sustained ventricular arrhythmias in whom no causative mutation was identified using a targeted gene panel including 28 genes. Methods and results: WES was applied on 2 affected cousins. Stringent filtering of the identified genetic variants was performed including population variant frequencies, in silico analysis, orthologous and paralogous conservation. Subsequently Sanger sequencing was performed for 10 potential disease causing variants in order to confirm the presence of the variant and to evaluate co-segregation. Only one variant in exon 9 of the RBM20 gene (c.2714T > A, p.Met950Lys, NM_001334363) showed full co-segregation in the 7 affected family members resulting in a maximum 2-point LOD score of 2.1 and suggesting this as the pathogenic mutation responsible for the phenotype. Recently mutations in RBM20 have been linked to arrhythmogenic dilated cardiomyopathy caused by defective splicing of the giant sarcomere protein titin and abnormal calcium handling. Conclusions: We report the identification of a novel mutation in RBM20 by WES in a large pedigree with DCM. [ABSTRACT FROM AUTHOR]

Published

2020

5. Pathogenic P554S Variant in TLR3 in a Patient with Severe Influenza Pneumonia.

Author

Bucciol, Giorgia, Desmet, Lars, Leuven Laboratory of Inborn Errors of Immunity, Moens, Leen, Delafontaine, Selket, Corveleyn, Anniek, and Meyts, Isabelle

Subjects

INFLUENZA, PNEUMONIA, CONTINUOUS positive airway pressure

Abstract

These patients and the patients reported by Lim et al. did not suffer from HSE or other severe viral infections, despite positive HSV serology in at least one patient, nor did our patient and her father, who is asymptomatic. Recently, Lim et al. described three unrelated children with influenza-related acute respiratory distress syndrome carrying the heterozygous loss of function I TLR3 i mutations P554S (dominant negative effect, two patients) and P680L (haploinsufficiency, one patient) [[3]]. TLR3 deficiency was also described in a patient suffering from recurrent HSV-triggered erythema multiforme and in patients suffering from severe influenza pneumonia [[2]]. [Extracted from the article]

Published

2022

6. Adult-Onset ANCA-Associated Vasculitis in SAVI: Extension of the Phenotypic Spectrum, Case Report and Review of the Literature.

Author

Staels, Frederik, Betrains, Albrecht, Doubel, Peter, Willemsen, Mathijs, Cleemput, Vincent, Vanderschueren, Steven, Corveleyn, Anniek, Meyts, Isabelle, Sprangers, Ben, Crow, Yanick J., Humblet-Baron, Stephanie, Liston, Adrian, and Schrijvers, Rik

Subjects

VASCULITIS, LITERATURE reviews, PULMONARY fibrosis, GAIN-of-function mutations, RENAL fibrosis, LEUKOCYTOCLASTIC vasculitis

Abstract

STING-associated vasculopathy with onset in infancy (SAVI) is an autosomal dominant disorder due to gain-of-function mutations in STING1 , also known as TMEM173 , encoding for STING. It was reported as a vasculopathy of infancy. However, since its description a wider spectrum of associated manifestations and disease-onset has been observed. We report a kindred with a heterozygous STING mutation (p.V155M) in which the 19-year-old proband suffered from isolated adult-onset ANCA-associated vasculitis. His father suffered from childhood-onset pulmonary fibrosis and renal failure attributed to ANCA-associated vasculitis, and died at the age of 30 years due to respiratory failure. In addition, an overview of the phenotypic spectrum of SAVI is provided highlighting (a) a high phenotypic variability with in some cases isolated manifestations, (b) the potential of adult-onset disease, and (c) a novel manifestation with ANCA-associated vasculitis. [ABSTRACT FROM AUTHOR]

Published

2020

7. Mutations in MAGT1 lead to a glycosylation disorder with a variable phenotype.

Author

Blommaert, Eline, Péanne, Romain, Cherepanova, Natalia A., Rymen, Daisy, Staels, Frederik, Jaeken, Jaak, Race, Valérie, Keldermans, Liesbeth, Souche, Erika, Corveleyn, Anniek, Sparkes, Rebecca, Bhattacharya, Kaustuv, Devalck, Christine, Schrijvers, Rik, Foulquier, François, Gilmore, Reid, and Matthijs, Gert

Subjects

GENETIC mutation, GLYCOSYLATION, PHENOTYPES, OLIGOSACCHARYLTRANSFERASE, TRANSFERRIN, CONGENITAL disorders

Abstract

Congenital disorders of glycosylation (CDG) are a group of rare metabolic diseases, due to impaired protein and lipid glycosylation. We identified two patients with defective serum transferrin glycosylation and mutations in the MAGT1 gene. These patients present with a phenotype that is mainly characterized by intellectual and developmental disability. MAGT1 has been described to be a subunit of the oligosaccharyltransferase (OST) complex and more specifically of the STT3B complex. However, it was also claimed that MAGT1 is a magnesium (Mg2+) transporter. So far, patients with mutations in MAGT1 were linked to a primary immunodeficiency, characterized by chronic EBV infections attributed to a Mg2+ homeostasis defect (XMEN). We compared the clinical and cellular phenotype of our two patients to that of an XMEN patient that we recently identified. All three patients have an N-glycosylation defect, as was shown by the study of different substrates, such as GLUT1 and SHBG, demonstrating that the posttranslational glycosylation carried out by the STT3B complex is dysfunctional in all three patients. Moreover, MAGT1 deficiency is associated with an enhanced expression of TUSC3, the homolog protein of MAGT1, pointing toward a compensatory mechanism. Hence, we delineate MAGT1-CDG as a disorder associated with two different clinical phenotypes caused by defects in glycosylation. [ABSTRACT FROM AUTHOR]

Published

2019

8. Human DOCK2 Deficiency: Report of a Novel Mutation and Evidence for Neutrophil Dysfunction.

Author

Moens, Leen, Gouwy, Mieke, Bosch, Barbara, Pastukhov, Oleksandr, Nieto-Patlàn, Alejandro, Siler, Ulrich, Bucciol, Giorgia, Mekahli, Djalila, Vermeulen, François, Desmet, Lars, Maebe, Sophie, Flipts, Helena, Corveleyn, Anniek, Moshous, Despina, Philippet, Pierre, Tangye, Stuart G., Boisson, Bertrand, Casanova, Jean-Laurent, Florkin, Benoit, and Struyf, Sofie

Subjects

NEUTROPHIL immunology, SEVERE combined immunodeficiency, KILLER cells, CELL migration, CYTOSKELETON, REACTIVE oxygen species

Abstract

DOCK2 is a guanine-nucleotide-exchange factor for Rac proteins. Activated Rac serves various cellular functions including the reorganization of the actin cytoskeleton in lymphocytes and neutrophils and production of reactive oxygen species in neutrophils. Since 2015, six unrelated patients with combined immunodeficiency and early-onset severe viral infections caused by bi-allelic loss-of-function mutations in DOCK2 have been described. Until now, the function of phagocytes, specifically neutrophils, has not been assessed in human DOCK2 deficiency. Here, we describe a new kindred with four affected siblings harboring a homozygous splice-site mutation (c.2704-2 A > C) in DOCK2. The mutation results in alternative splicing and a complete loss of DOCK2 protein expression. The patients presented with leaky severe combined immunodeficiency or Omenn syndrome. The novel mutation affects EBV-B cell migration and results in NK cell dysfunction similar to previous observations. Moreover, both cytoskeletal rearrangement and reactive oxygen species production are partially impaired in DOCK2-deficient neutrophils. [ABSTRACT FROM AUTHOR]

Published

2019

9. Pathogenic TLR3 Variant in a Patient with Recurrent Herpes Simplex Virus 1–Triggered Erythema Multiforme.

Author

Bucciol, Giorgia, Delafontaine, Selket, Moens, Leen, Corveleyn, Anniek, Morren, Marie-Anne, and Meyts, Isabelle

Subjects

HERPES simplex virus, ERYTHEMA multiforme, TOXIC epidermal necrolysis, DIAGNOSIS, HEALING, SYMPTOMS

Abstract

First, in HSV-associated EM, HSV-1 viral genes are expressed in intralesional keratinocytes and drive T helper 1-mediated inflammatory responses [[9]]. 1:CAS:528:DC%2BC3cXovFels7g%3D. 10.1074/jbc.M109.047464 9 Gober MD, Laing JM, Burnett JW, Aurelian L. The herpes simplex virus gene pol expressed in herpes-associated erythema multiforme lesions upregulates/activates SP1 and inflammatory cytokines. 1:CAS:528:DC%2BD2sXos1Kns7c%3D. 10.1159/000104259 10 Aurelian L, Ono F, Burnett J. Herpes simplex virus (HSV)-associated erythema multiforme (HAEM): a viral disease with an autoimmune component. [Extracted from the article]

Published

2021

10. Genotype-phenotype relationship and risk stratification in loss-of-function SCN5A mutation carriers.

Author

Robyns, Tomas, Nuyens, Dieter, Vandenberk, Bert, Kuiperi, Cuno, Corveleyn, Anniek, Breckpot, Jeroen, Garweg, Christophe, Ector, Joris, and Willems, Rik

Abstract

Introduction: Loss-of-function (LoF) mutations in the SCN5A gene cause multiple phenotypes including Brugada Syndrome (BrS) and a diffuse cardiac conduction defect. Markers of increased risk for sudden cardiac death (SCD) in LoF SCN5A mutation carriers are ill defined. We hypothesized that late potentials and fragmented QRS would be more prevalent in SCN5A mutation carriers compared to SCN5A-negative BrS patients and evaluated risk markers for SCD in SCN5A mutation carriers.Methods: We included all SCN5A loss-of-function mutation carriers and SCN5A-negative BrS patients from our center. A combined arrhythmic endpoint was defined as appropriate ICD shock or SCD.Results: Late potentials were more prevalent in 79 SCN5A mutation carriers compared to 39 SCN5A-negative BrS patients (66% versus 44%, p = .021), while there was no difference in the prevalence of fragmented QRS. PR interval prolongation was the only parameter that predicted the presence of a SCN5A mutation in BrS (OR 1.08; p < .001). Four SCN5A mutation carriers, of whom three did not have a diagnostic type 1 ECG either spontaneously or after provocation with a sodium channel blocker, reached the combined arrhythmic endpoint during a follow-up of 44 ± 52 months resulting in an annual incidence rate of 1.37%.Conclusion: LP were more frequently observed in SCN5A mutation carriers, while fQRS was not. In SCN5A mutation carriers, the annual incidence rate of SCD was non-negligible, even in the absence of a spontaneous or induced type 1 ECG. Therefore, proper follow-up of SCN5A mutation carriers without Brugada syndrome phenotype is warranted. [ABSTRACT FROM AUTHOR]

Published

2018

11. A comprehensive clinical and genetic study in 127 patients with ID in Kinshasa, DR Congo.

Author

Lumaka, Aimé, Race, Valerie, Peeters, Hilde, Corveleyn, Anniek, Coban‐Akdemir, Zeynep, Jhangiani, Shalini N., Song, Xiaofei, Mubungu, Gerrye, Posey, Jennifer, Lupski, James R., Vermeesch, Joris R., Lukusa, Prosper, and Devriendt, Koenraad

Abstract

Pathogenic variants account for 4 to 41% of patients with intellectual disability (ID) or developmental delay (DD). In Sub‐Saharan Africa, the prevalence of ID is thought to be higher, but data in Central Africa are limited to some case reports. In addition, clinical descriptions of some syndromes are not available for this population. This study aimed at providing an estimate for the fraction of ID/DD for which an underlying etiological genetic cause may be elucidated and provide insights into their clinical presentation in special institutions in a Central African country. A total of 127 patients (33 females and 94 males, mean age 10.03 ± 4.68 years), were recruited from six institutions across Kinshasa. A clinical diagnosis was achieved in 44 but molecular confirmation was achieved in 21 of the 22 patients with expected genetic defect (95% clinical sensitivity). Identified diseases included Down syndrome (15%), submicroscopic copy number variants (9%), aminoacylase deficiency (0.8%), Partington syndrome in one patient (0.8%) and his similarly affected brother, X‐linked syndromic Mental Retardation type 33 (0.8%), and two conditions without clear underlying molecular genetic etiologies (Oculo‐Auriculo‐Vertebral and Amniotic Bands Sequence). We have shown that genetic etiologies, similar to those reported in Caucasian subjects, are a common etiologic cause of ID in African patients from Africa. We have confirmed the diagnostic utility of clinical characterization prior to genetic testing. Finally, our clinical descriptions provide insights into the presentation of these genetic diseases in African patients. [ABSTRACT FROM AUTHOR]

Published

2018

12. Discordance for placental mesenchymal dysplasia in a monochorionic diamniotic twin pregnancy: A case report.

Author

Gheysen, Willem, Strybol, David, Moerman, Philippe, Steylemans, An, Corveleyn, Anniek, De Catte, Luc, Couck, Isabel, and Lewi, Liesbeth

Subjects

DYSPLASIA, TWINS, PREGNANCY complications, ULTRASONIC imaging, KARYOTYPES, DIAGNOSIS

Abstract

Key Clinical Message: Placental mesenchymal dysplasia (PMD) occurs in about 1 in 5000 pregnancies. The differential diagnosis between PMD and partial mole is difficult on ultrasound scan, and karyotyping plays a key role in distinguishing PMD from partial mole. Our report is the first to report on the discordancy for PMD in a monochorionic setting. [ABSTRACT FROM AUTHOR]

Published

2018

13. Compound heterozygous loss-of-function mutations in KIF20A are associated with a novel lethal congenital cardiomyopathy in two siblings.

Author

Louw, Jacoba J., Nunes Bastos, Ricardo, Chen, Xiaowen, Verdood, Céline, Corveleyn, Anniek, Jia, Yaojuan, Breckpot, Jeroen, Gewillig, Marc, Peeters, Hilde, Santoro, Massimo M., Barr, Francis, and Devriendt, Koenraad

Subjects

CARDIOMYOPATHIES, CONGENITAL disorders, AUTOSOMAL recessive polycystic kidney, SINGLE nucleotide polymorphisms, EXOMES

Abstract

Congenital or neonatal cardiomyopathies are commonly associated with a poor prognosis and have multiple etiologies. In two siblings, a male and female, we identified an undescribed type of lethal congenital restrictive cardiomyopathy affecting the right ventricle. We hypothesized a novel autosomal recessive condition. To identify the cause, we performed genetic, in vitro and in vivo studies. Genome-wide SNP typing and parametric linkage analysis was done in a recessive model to identify candidate regions. Exome sequencing analysis was done in unaffected and affected siblings. In the linkage regions, we selected candidate genes that harbor two rare variants with predicted functional effects in the patients and for which the unaffected sibling is either heterozygous or homozygous reference. We identified two compound heterozygous variants in KIF20A; a maternal missense variant (c.544C>T: p.R182W) and a paternal frameshift mutation (c.1905delT: p.S635Tfs*15). Functional studies confirmed that the R182W mutation creates an ATPase defective form of KIF20A which is not able to support efficient transport of Aurora B as part of the chromosomal passenger complex. Due to this, Aurora B remains trapped on chromatin in dividing cells and fails to translocate to the spindle midzone during cytokinesis. Translational blocking of KIF20A in a zebrafish model resulted in a cardiomyopathy phenotype. We identified a novel autosomal recessive congenital restrictive cardiomyopathy, caused by a near complete loss-of-function of KIF20A. This finding further illustrates the relationship of cytokinesis and congenital cardiomyopathy. [ABSTRACT FROM AUTHOR]

Published

2018

14. PID in Disguise: Molecular Diagnosis of IRAK-4 Deficiency in an Adult Previously Misdiagnosed With Autosomal Dominant Hyper IgE Syndrome.

Author

Frans, Glynis, Moens, Leen, Schrijvers, Rik, Wuyts, Greet, Bouckaert, Bernard, Schaballie, Heidi, Dupont, Lieven, Bossuyt, Xavier, Corveleyn, Anniek, and Meyts, Isabelle

Subjects

INTERLEUKIN-1 receptors, IMMUNODEFICIENCY, IMMUNOGLOBULIN E, DIAGNOSTIC errors, T helper cells, DIAGNOSIS

Abstract

Autosomal recessive IL-1R-associated kinase 4 (IRAK-4) deficiency is a rare cause of recurrent pyogenic infections with limited inflammatory responses. We describe an adult female patient with severe lung disease who was phenotypically diagnosed as suffering from autosomal dominant Hyper IgE syndrome (AD HIES) because of recurrent skin infections with Staphylococcus aureus, recurrent pneumonia and elevated serum IgE levels. In contrast to findings in AD HIES patients, no abnormalities were found in the Th17 and circulating follicular helper T cell subsets. A panel-based sequencing approach led to the identification of a homozygous IRAK4 stop mutation (c.877C > T, p.Gln293*). [ABSTRACT FROM AUTHOR]

Published

2015

15. The diagnostic value of next generation sequencing in familial nonsyndromic congenital heart defects.

Author

Jia, Yaojuan, Louw, Jacoba J., Breckpot, Jeroen, Callewaert, Bert, Barrea, Catherine, Sznajer, Yves, Gewillig, Marc, Souche, Erika, Dehaspe, Luc, Vermeesch, Joris Robert, Lambrechts, Diether, Devriendt, Koenraad, and Corveleyn, Anniek

Abstract

To determine the diagnostic value of massive parallel sequencing of a panel of known cardiac genes in familial nonsyndromic congenital heart defects (CHD), targeted sequencing of the coding regions of 57 genes previously implicated in CHD was performed in 36 patients from 13 nonsyndromic CHD families with probable autosomal dominant inheritance. Following variant analysis and Sanger validation, we identified six potential disease causing variants in three genes ( MYH6, NOTCH1, and TBX5), which may explain the defects in six families. Several problematic situations were encountered when performing genotype-phenotype correlations in the families to confirm the causality of these variants. In conclusion, by screening known CHD-associated genes in well-selected nonsyndromic CHD families and cautious variant interpretation, potential causative variants were identified in less than half of the families (6 out of 13; 46%). Variant interpretation remains a major challenge reflecting the complex genetic cause of CHD. 2015 Wiley Periodicals, Inc. [ABSTRACT FROM AUTHOR]

Published

2015

16. MEIS2 involvement in cardiac development, cleft palate, and intellectual disability.

Author

Louw, Jacoba J., Corveleyn, Anniek, Jia, Yaojuan, Hens, Greet, Gewillig, Marc, and Devriendt, Koenraad

Abstract

MEIS2 has been associated with cleft palate and cardiac septal defects as well as varying degrees of intellectual disability. We present a female patient with a more severe phenotype compared to previous reported patients. She has multiple congenital malformations; cleft palate and congenital heart defect characterized by septal defects and aortic coarctation. She has severe feeding problems, facial dysmorphism, severely delayed gross motor and verbal development, and autism spectrum disorder. Facial dysmorphism consisting of bitemporal narrowing, arched and laterally extended eyebrows, mild upslanting palpebral fissures, deep-set eyes, a tented upper lip, thin upper vermilion, full lower vermilion, broad first ray of hands and feet, a gap between the first and second toes, and syndactyly of toe II-III. Exome sequencing revealed a non-frameshift deletion (c.998_1000del:p.Arg333del) of three base pairs in the MEIS2 homeodomain. The more severe phenotype is most probably due to dominant-negative mechanisms. This is the first report showing a de novo small intragenic mutation in MEIS2 and further confirms the important role of this gene in normal development. © 2015 Wiley Periodicals, Inc. [ABSTRACT FROM AUTHOR]

Published

2015

17. Criteria for HNF1B analysis in patients with congenital abnormalities of kidney and urinary tract.

Author

Raaijmakers, Anke, Corveleyn, Anniek, Devriendt, Koen, van Tienoven, Theun Pieter, Allegaert, Karel, Van Dyck, Mieke, van den Heuvel, Lambertus, Kuypers, Dirk, Claes, Kathleen, Mekahli, Djalila, and Levtchenko, Elena

Subjects

HEPATOCYTE nuclear factors, HUMAN abnormalities, KIDNEY diseases, URINARY tract infections, KIDNEY development, PATIENTS

Abstract

Background. Congenital anomalies of kidneys and urinary tract (CAKUT) are the most predominant developmental disorders comprising ~20-30% of all anomalies identified in the prenatal period. Mutations in hepatocyte nuclear factor 1-beta (HNF-1ß) involved in the development of kidneys, liver, pancreas and urogenital tract are currently the most frequent monogenetic cause of CAKUT found in 10-30% of patients depending on screening policy and study design. We aimed to validate criteria for analysis of HNF1B in a prospective cohort of paediatric and adult CAKUT patients. Methods. We included CAKUT patients diagnosed in our paediatric and adult nephrology departments from January 2010 until April 2013 based on predefined screening criteria. Subjects presenting with at least one major renal criterion or one minor renal criterion combined with one or more extrarenal criteria in the personal history or a familial history of renal or extra-renal manifestations were considered eligible. Results. We prospectively screened 205 patients and detected HNF1B mutations in 10% [n = 20, 12 children, median age 4.2 (range 0-13.1) years and 8 adults, median age 34.8 (range 16.6-62) years]. We observed that bilateral renal anomaly, renal cysts from unknown origin, a combination of two major renal anomalies and hypomagnesaemia were predictive for finding HNF1B mutations (P < 0.001; P < 0.001; P = 0.004; P = 0.008, respectively). Conclusions. We demonstrated that HNF1B mutations are responsible for ~10% of CAKUT cases, both in children and in adults. Based on our results we propose adapted criteria for HNF1B analysis to reduce the screening costs without missing affected patients. These criteria should be reaffirmed in a larger validation cohort. [ABSTRACT FROM AUTHOR]

Published

2015

18. Heterozygous [alpha]1-antitrypsin Z allele mutation in presumed healthy donor livers used for transplantation.

Author

Roelandt, Philip, Dobbels, Pieter, Komuta, Mina, Corveleyn, Anniek, Emonds, Marie-Paule, Roskams, Tania, Aerts, Raymond, Monbaliu, Diethard, Libbrecht, Louis, Laleman, Wim, Verslype, Chris, Van Steenbergen, Werner, van der Merwe, Schalk, Pirenne, Jacques, Nevens, Frederik, and Cassiman, David

Published

2013

19. Misdiagnosis as asphyxiating thoracic dystrophy and CMV-associated haemophagocytic lymphohistiocytosis in Shwachman-Diamond syndrome.

Author

Schaballie, Heidi, Renard, Marleen, Vermylen, Christiane, Scheers, Isabelle, Revencu, Nicole, Regal, Luc, Cassiman, David, Sevenants, Lieve, Hoffman, Ilse, Corveleyn, Anniek, Bordon, Victoria, Haerynck, Filomeen, Allegaert, Karel, Boeck, Kris, Roskams, Tania, Boeckx, Nancy, Bossuyt, Xavier, and Meyts, Isabelle

Subjects

SHWACHMAN-Diamond Syndrome, BONE marrow diseases, MACROPHAGES, CYTOMEGALOVIRUS disease diagnosis, IMMUNOLOGIC diseases, HEPATOPULMONARY syndrome, DIAGNOSIS

Abstract

Shwachman-Diamond syndrome (SDS) is an autosomal recessive disorder characterised by skeletal dysplasia, exocrine pancreatic insufficiency and bone marrow failure. Various other conditions, such as hepatopathy and failure to thrive have been associated with SDS. A retrospective study was conducted to describe mutations, clinical features, and the immunological profile of 11 Belgian patients with genetically confirmed diagnosis of SDS. This study confirms the existing understanding of the classical features of SDS although the typical triad was present in only six out of nine fully studied patients. The following important observations are made in this cohort. Four out of eleven patients were misdiagnosed as having Asphyxiating Thoracic Dystrophy (Jeune syndrome) because of severe thoracic dystrophy. Another two patients presented with unexplained episodes of symptomatic hypoglycaemia. The immunological phenotype was heterogeneous although laboratory abnormalities were noticed in eight out of ten patients assessed. Three patients experienced a life threatening viral infection (respiratory syncytial virus, cytomegalovirus (CMV) and rotavirus). In one patient, CMV infection caused an episode of haemophagocytic lymphohistiocytosis. One patient has bronchiectasis at the age of 3 years due to recurrent respiratory tract infections. These findings strengthen the suspicion of an abnormal immune system in SDS. Liver anomalies, usually described as benign and transitory in SDS patients, were severe in two patients of the cohort. One patient developed hepatopulmonary syndrome. The findings in this national cohort of SDS patients could contribute to the prevention of misdiagnosis in the future and enable more rapid recognition of certain severe complications. [ABSTRACT FROM AUTHOR]

Published

2013

20. Novel COL4A1 mutations cause cerebral small vessel disease by haploinsufficiency.

Author

Lemmens, Robin, Maugeri, Alessandra, Niessen, Hans W. M., Goris, An, Tousseyn, Thomas, Demaerel, Philippe, Corveleyn, Anniek, Robberecht, Wim, van der Knaap, Marjo S., Thijs, Vincent N., and Zwijnenburg, Petra J.G.

Published

2013

21. A standardized framework for the validation and verification of clinical molecular genetic tests.

Author

Mattocks, Christopher J., Morris, Michael A., Matthijs, Gert, Swinnen, Elfriede, Corveleyn, Anniek, Dequeker, Els, Müller, Clemens R., Pratt, Victoria, and Wallace, Andrew

Subjects

HUMAN chromosome abnormality diagnosis, HUMAN molecular genetics, MEDICAL personnel, LABORATORIES, VALIDATION therapy

Abstract

The validation and verification of laboratory methods and procedures before their use in clinical testing is essential for providing a safe and useful service to clinicians and patients. This paper outlines the principles of validation and verification in the context of clinical human molecular genetic testing. We describe implementation processes, types of tests and their key validation components, and suggest some relevant statistical approaches that can be used by individual laboratories to ensure that tests are conducted to defined standards. [ABSTRACT FROM AUTHOR]

Published

2010

22. Provision and quality assurance of preimplantation genetic diagnosis in Europe.

Author

Corveleyn, Anniek, Morris, Michael A, Dequeker, Elisabeth, Sermon, Karen, Davies, James Lawford, Antiñolo, Guillermo, Schmutzler, Andreas, Vanecek, Jiri, Nagels, Nick, Zika, Eleni, Palau, Francesc, and Ibarreta, Dolores

Subjects

PREIMPLANTATION genetic diagnosis, HUMAN reproductive technology, HUMAN genetics, QUALITY assurance

Abstract

Preimplantation genetic diagnosis (PGD) is now well established and provided in many European countries. However, regulations, professional standards and accreditation requirements can differ notably. Furthermore, no comprehensive independent data exist either about practice and provision in Europe or about the quality assurance practices and procedures designed to optimize the quality of the results. Consequently, a study was launched to obtain knowledge, currently lacking, of the provision and quality assurance of PGD services and cross-border activities in Europe. An online questionnaire was developed and sent to PGD providers, and expert opinions were obtained through interviews with professionals in specific countries. Information was gathered from 53 centres offering PGD in 17 European countries. There is a diverse array of tests available, with a trend for custom-made services. Although half of the centres have a designated quality manager, just 33% have achieved or are preparing for accreditation or certification. About 66% of the centres responded that they did not participate in external quality assessment, a problem exacerbated by the lack of existing PGD-specific schemes. Approximately 19% of the centres do not keep data on accuracy and 9% do not even follow up until birth. PGD is an expanding activity with an increasing international flow that accounts for approximately one-third of the activity reported. The survey highlights a significant need for improvement in quality assurance in PGD centres. On the positive side, important improvements in the quality management of these services are expected with the European Tissue Directive entering into force.European Journal of Human Genetics (2008) 16, 290–299; doi:10.1038/sj.ejhg.5201976; published online 19 December 2007 [ABSTRACT FROM AUTHOR]

Published

2008

23. Targeted capture sequencing in a large LQTS family reveals a new pathogenic mutation c.2038delG in KCNH2 initially missed due to allelic dropout.

Author

ROBYNS, Tomas, KUIPERI, Cuno, WILLEMS, Rik, CORVELEYN, Anniek, and NUYENS, Dieter

Abstract

We present a new mutation in KCNH2 (c.2038delG) resulting in a frameshift and premature truncation of the IKr channel protein in a large LQTS family with several sudden death cases. This mutation was initially missed by mutation scanning with DHPLC due to allelic dropout and only retrieved after repeat genetic testing with targeted capture and massive parallel sequencing. There was full penetrance of this mutation, only if an individualized QT correction derived from 24-hour Holter data was used. This case again underscores the importance of repeat genetic testing in robust cases of LQTS that remained genotype negative with mutation scanning techniques. [ABSTRACT FROM AUTHOR]

Published

2015