Your search keyword '"Mortier, G."' showing total 9 results

1. Resequencing of candidate genes for Keratoconus reveals a role for Ehlers-Danlos Syndrome genes.

Author

Fransen E, Valgaeren H, Janssens K, Sommen M, De Ridder R, Vandeweyer G, Bisceglia L, Soler V, Hoischen A, Mortier G, Malecaze F, Koppen C, and Van Camp G

Subjects

Collagen Type II genetics, Collagen Type V genetics, Ehlers-Danlos Syndrome diagnosis, Humans, Keratoconus diagnosis, Sequence Analysis, DNA, Tenascin genetics, Transcription Factors genetics, Ehlers-Danlos Syndrome genetics, Keratoconus genetics

Abstract

The involvement of genetic factors in the pathogenesis of KC has long been recognized but the identification of variants affecting the underlying protein functions has been challenging. In this study, we selected 34 candidate genes for KC based on previous whole-exome sequencing (WES) and the literature, and resequenced them in 745 KC patients and 810 ethnically matched controls from Belgium, France and Italy. Data analysis was performed using the single variant association test as well as gene-based mutation burden and variance components tests. In our study, we detected enrichment of genetic variation across multiple gene-based tests for the genes COL2A1, COL5A1, TNXB, and ZNF469. The top hit in the single variant association test was obtained for a common variant in the COL12A1 gene. These associations were consistently found across independent subpopulations. Interestingly, COL5A1, TNXB, ZNF469 and COL12A1 are all known Ehlers-Danlos Syndrome (EDS) genes. Though the co-occurrence of KC and EDS has been reported previously, this study is the first to demonstrate a consistent role of genetic variants in EDS genes in the etiology of KC. In conclusion, our data show a shared genetic etiology between KC and EDS, and clearly confirm the currently disputed role of ZNF469 in disease susceptibility for KC., (© 2021. The Author(s), under exclusive licence to European Society of Human Genetics.)

Published

2021

2. Novel microdeletions on chromosome 14q32.2 suggest a potential role for non-coding RNAs in Kagami-Ogata syndrome.

Author

van der Werf IM, Buiting K, Czeschik C, Reyniers E, Vandeweyer G, Vanhaesebrouck P, Lüdecke HJ, Wieczorek D, Horsthemke B, Mortier G, Leroy JG, and Kooy RF

Subjects

Chromosome Disorders diagnosis, Chromosomes, Human, Pair 14 genetics, Humans, Pedigree, Phenotype, Syndrome, Uniparental Disomy diagnosis, Chromosome Disorders genetics, RNA, Untranslated genetics, Sequence Deletion, Uniparental Disomy genetics

Abstract

In approximately 20% of individuals with Kagami-Ogata syndrome (KOS14, MIM 608149), characterized by a bell-shaped thorax with coat-hanger configuration of the ribs, joint contractures, abdominal wall defects and polyhydramnios during the pregnancy, the syndrome is caused by a maternal deletion of the imprinted gene cluster in chromosome 14q32.2. Most deletions reported so far included one or both of the differentially methylated regions (DMRs) - DLK1/MEG3 IG-DMR and MEG3-DMR. We present two unrelated families with two affected siblings each, presenting with classical KOS14 due to maternally inherited microdeletions. Interestingly, all four patients have lived through to adulthood, even though mortality rates for patients with KOS14 due to a microdeletion are relatively high. In the first family, none of the DMRs is included in the deletion and the methylation status is identical to that of controls. Deletions that do not encompass the DMRs in this region are thus sufficient to elicit the full KOS14 phenotype. In the second family, a partially overlapping deletion including both DMRs and MEG3 was detected. In summary, we show that patients with KOS14 can live into adulthood, that causal deletions do not have to include the DMRs and that consequently a normal methylation pattern does not exclude KOS14.

Published

2016

3. A catalog of hemizygous variation in 127 22q11 deletion patients.

Author

Hestand MS, Nowakowska BA, Vergaelen E, Van Houdt J, Dehaspe L, Suhl JA, Del-Favero J, Mortier G, Zackai E, Swillen A, Devriendt K, Gur RE, McDonald-McGinn DM, Warren ST, Emanuel BS, and Vermeesch JR

Abstract

The 22q11.2 deletion syndrome is the most common microdeletion disorder, with wide phenotypic variability. To investigate variation within the non-deleted allele we performed targeted resequencing of the 22q11.2 region for 127 patients, identifying multiple deletion sizes, including two deletions with atypical breakpoints. We cataloged ~12,000 hemizygous variant positions, of which 84% were previously annotated. Within the coding regions 95 non-synonymous variants, three stop gains, and two frameshift insertions were identified, some of which we speculate could contribute to atypical phenotypes. We also catalog tolerability of 22q11 gene mutations based on related autosomal recessive disorders in man, embryonic lethality in mice, cross-species conservation and observations that some genes harbor more or less variants than expected. This extensive catalog of hemizygous variants will serve as a blueprint for future experiments to correlate 22q11DS variation with phenotype.

Published

2016

4. Mate pair sequencing for the detection of chromosomal aberrations in patients with intellectual disability and congenital malformations.

Author

Vergult S, Van Binsbergen E, Sante T, Nowak S, Vanakker O, Claes K, Poppe B, Van der Aa N, van Roosmalen MJ, Duran K, Tavakoli-Yaraki M, Swinkels M, van den Boogaard MJ, van Haelst M, Roelens F, Speleman F, Cuppen E, Mortier G, Kloosterman WP, and Menten B

Subjects

Abnormalities, Multiple diagnosis, Chromosome Banding, Chromosome Duplication, Chromosomes, Human, Pair 18, Chromosomes, Human, Pair 21, Comparative Genomic Hybridization, Computational Biology, Female, Humans, Intellectual Disability diagnosis, Karyotype, Male, Recombination, Genetic, Abnormalities, Multiple genetics, Chromosome Aberrations, High-Throughput Nucleotide Sequencing, Intellectual Disability genetics

Abstract

Recently, microarrays have replaced karyotyping as a first tier test in patients with idiopathic intellectual disability and/or multiple congenital abnormalities (ID/MCA) in many laboratories. Although in about 14-18% of such patients, DNA copy-number variants (CNVs) with clinical significance can be detected, microarrays have the disadvantage of missing balanced rearrangements, as well as providing no information about the genomic architecture of structural variants (SVs) like duplications and complex rearrangements. Such information could possibly lead to a better interpretation of the clinical significance of the SV. In this study, the clinical use of mate pair next-generation sequencing was evaluated for the detection and further characterization of structural variants within the genomes of 50 ID/MCA patients. Thirty of these patients carried a chromosomal aberration that was previously detected by array CGH or karyotyping and suspected to be pathogenic. In the remaining 20 patients no causal SVs were found and only benign aberrations were detected by conventional techniques. Combined cluster and coverage analysis of the mate pair data allowed precise breakpoint detection and further refinement of previously identified balanced and (complex) unbalanced aberrations, pinpointing the causal gene for some patients. We conclude that mate pair sequencing is a powerful technology that can provide rapid and unequivocal characterization of unbalanced and balanced SVs in patient genomes and can be essential for the clinical interpretation of some SVs.

Published

2014

5. 17q24.2 microdeletions: a new syndromal entity with intellectual disability, truncal obesity, mood swings and hallucinations.

Author

Vergult S, Dauber A, Delle Chiaie B, Van Oudenhove E, Simon M, Rihani A, Loeys B, Hirschhorn J, Pfotenhauer J, Phillips JA 3rd, Mohammed S, Ogilvie C, Crolla J, Mortier G, and Menten B

Subjects

Child, Child, Preschool, Female, Humans, Irritable Mood, MicroRNAs metabolism, Protein Kinase C-alpha genetics, Seizures genetics, Syndrome, Young Adult, Chromosome Deletion, Chromosomes, Human, Pair 17 genetics, Hallucinations genetics, Intellectual Disability genetics, Obesity, Abdominal genetics

Abstract

Although microdeletions of the long arm of chromosome 17 are being reported with increasing frequency, deletions of chromosome band 17q24.2 are rare. Here we report four patients with a microdeletion encompassing chromosome band 17q24.2 with a smallest region of overlap of 713 kb containing five Refseq genes and one miRNA. The patients share the phenotypic characteristics, such as intellectual disability (4/4), speech delay (4/4), truncal obesity (4/4), seizures (2/4), hearing loss (3/4) and a particular facial gestalt. Hallucinations and mood swings were also noted in two patients. The PRKCA gene is a very interesting candidate gene for many of the observed phenotypic features, as this gene plays an important role in many cellular processes. Deletion of this gene might explain the observed truncal obesity and could also account for the hallucinations and mood swings seen in two patients, whereas deletion of a CACNG gene cluster might be responsible for the seizures observed in two patients. In one of the patients, the PRKAR1A gene responsible for Carney Complex and the KCNJ2 gene causal for Andersen syndrome are deleted. This is the first report of a patient with a whole gene deletion of the KCNJ2 gene.

Published

2012

6. Nasal speech and hypothyroidism are common hallmarks of 12q15 microdeletions.

Author

Vergult S, Krgovic D, Loeys B, Lyonnet S, Liedén A, Anderlid BM, Sharkey F, Joss S, Mortier G, and Menten B

Subjects

Adult, Child, Chromosome Disorders genetics, Developmental Disabilities genetics, Female, Genetic Association Studies, Humans, Hypothyroidism genetics, Male, Young Adult, Chromosome Deletion, Chromosome Disorders pathology, Chromosomes, Human, Pair 12 genetics, Developmental Disabilities pathology, Hypothyroidism pathology, Speech physiology

Abstract

The introduction of array CGH in clinical diagnostics has led to the discovery of many new microdeletion/microduplication syndromes. Most of them are rare and often present with a variable range of clinical anomalies. In this study we report three patients with a de novo overlapping microdeletion of chromosome bands 12q15q21.1. The deletions are ∼2.5 Mb in size, with a 1.34-Mb common deleted region containing six RefSeq genes. All three patients present with learning disability or developmental delay, nasal speech and hypothyroidism. In this paper we will further elaborate on the genotype-phenotype correlation associated with this deletion and compare our patients with previously reported cases.

Published

2011

7. Perinatal/neonatal case presentation: unexpected severe respiratory insufficiency in a newborn with Holt-Oram Syndrome.

Author

Smets K, Mortier G, and Zecic A

Subjects

Cardiomegaly complications, Carpal Bones abnormalities, Finger Phalanges abnormalities, Heart Defects, Congenital genetics, Humans, Infant, Newborn, Lung abnormalities, Respiration, Artificial, Respiratory Insufficiency genetics, Syndrome, T-Box Domain Proteins genetics, Hand Bones abnormalities, Heart Defects, Congenital complications, Radius abnormalities, Respiratory Insufficiency etiology

Abstract

Holt-Oram syndrome is an autosomal dominant condition characterized by skeletal and cardiac defects. Pulmonary malformation is not reported to belong to the spectrum of this condition. We report a second case of a newborn with Holt-Oram syndrome who developed severe respiratory insufficiency shortly after birth. We discuss possible genetic links between abnormal pulmonary morphogenesis and Holt-Oram syndrome., (Journal of Perinatology (2005) 25, 745-746. doi:10.1038/sj.jp.7211384.)

Published

2005

8. Minimum prevalence, birth incidence and cause of death for Prader-Willi syndrome in Flanders.

Author

Vogels A, Van Den Ende J, Keymolen K, Mortier G, Devriendt K, Legius E, and Fryns JP

Subjects

Adolescent, Adult, Age of Onset, Belgium epidemiology, Birth Rate, Child, Child, Preschool, Female, Humans, Incidence, Infant, Infant, Newborn, Male, Middle Aged, Prader-Willi Syndrome diagnosis, Prevalence, Cause of Death, Prader-Willi Syndrome epidemiology, Prader-Willi Syndrome mortality

Abstract

The identification of all people with a diagnosis of Prader-Willi syndrome (PWS) confirmed by DNA methylation analysis living in Flanders was attempted through contact with the four genetic centres and the PWS Association. The birth incidence for the period 1993-2001 was 1:26 676, the minimum prevalence at 31 December 2001 was 1:76 574. A decreasing number of cases with age was found, which can be explained by a number of missing cases in the older population, a higher neonatal mortality in the past and an increasing mortality with age. Childhood death is usually sudden and associated with respiratory infection and high temperature, while the cause of death in adults is considered to be circulatory or respiratory in origin.

Published

2004

9. Clinical and radiographic features of multiple epiphyseal dysplasia not linked to the COMP or type IX collagen genes.

Author

Mortier GR, Chapman K, Leroy JL, and Briggs MD

Subjects

Adolescent, Adult, Cartilage growth & development, Cartilage Oligomeric Matrix Protein, Child, Child, Preschool, Female, Genetic Linkage, Humans, Infant, Knee Joint diagnostic imaging, Knee Joint pathology, Male, Matrilin Proteins, Middle Aged, Osteochondrodysplasias diagnostic imaging, Pedigree, Pelvis diagnostic imaging, Pelvis pathology, Radiography, Collagen genetics, Extracellular Matrix Proteins genetics, Glycoproteins genetics, Osteochondrodysplasias genetics, Osteochondrodysplasias pathology

Abstract

Multiple epiphyseal dysplasia (MED) is a mild chondrodysplasia affecting the structural integrity of cartilage and causing early-onset osteoarthrosis in adulthood. The condition is genetically heterogeneous. Mutations in the COMP gene and in two genes (COL9A2; COL9A3), coding respectively for the alpha2(IX) and alpha3(IX) chains of type IX collagen, can cause the autosomal dominant forms of MED. Mutations in the DTDST gene have recently been identified in a recessive form of MED. However, for the majority of MED cases, the genetic defect still remains undetermined. We report a three-generation family with an autosomal dominant form of MED, characterised by normal stature, joint pain in childhood and early-onset osteoarthrosis, affecting mainly the hips and knees. Based on discordant inheritance among affected individuals linkage of the phenotype to the COMP, COL9A1, COL9A2, COL9A3 genes was excluded. Our study provides evidence that at least another locus, distinct from COL9A1, is involved in autosomal dominant MED.

Published

2001