Your search keyword '"Corveleyn, Anniek"' showing total 3 results

1. Heterozygous loss-of-function variants of MEIS2 cause a triad of palatal defects, congenital heart defects, and intellectual disability.

Author

Verheije R, Kupchik GS, Isidor B, Kroes HY, Lynch SA, Hawkes L, Hempel M, Gelb BD, Ghoumid J, D'Amours G, Chandler K, Dubourg C, Loddo S, Tümer Z, Shaw-Smith C, Nizon M, Shevell M, Van Hoof E, Anyane-Yeboa K, Cerbone G, Clayton-Smith J, Cogné B, Corre P, Corveleyn A, De Borre M, Hjortshøj TD, Fradin M, Gewillig M, Goldmuntz E, Hens G, Lemyre E, Journel H, Kini U, Kortüm F, Le Caignec C, Novelli A, Odent S, Petit F, Revah-Politi A, Stong N, Strom TM, van Binsbergen E, Devriendt K, and Breckpot J

Subjects

Adolescent, Child, Child, Preschool, Cleft Palate pathology, Female, Heart Defects, Congenital pathology, Heterozygote, Homeodomain Proteins metabolism, Humans, Intellectual Disability pathology, Male, Phenotype, Syndrome, Transcription Factors metabolism, Young Adult, Cleft Palate genetics, Heart Defects, Congenital genetics, Homeodomain Proteins genetics, Intellectual Disability genetics, Loss of Function Mutation, Transcription Factors genetics

Abstract

Deletions on chromosome 15q14 are a known chromosomal cause of cleft palate, typically co-occurring with intellectual disability, facial dysmorphism, and congenital heart defects. The identification of patients with loss-of-function variants in MEIS2, a gene within this deletion, suggests that these features are attributed to haploinsufficiency of MEIS2. To further delineate the phenotypic spectrum of the MEIS2-related syndrome, we collected 23 previously unreported patients with either a de novo sequence variant in MEIS2 (9 patients), or a 15q14 microdeletion affecting MEIS2 (14 patients). All but one de novo MEIS2 variant were identified by whole-exome sequencing. One variant was found by targeted sequencing of MEIS2 in a girl with a clinical suspicion of this syndrome. In addition to the triad of palatal defects, heart defects, and developmental delay, heterozygous loss of MEIS2 results in recurrent facial features, including thin and arched eyebrows, short alae nasi, and thin vermillion. Genotype-phenotype comparison between patients with 15q14 deletions and patients with sequence variants or intragenic deletions within MEIS2, showed a higher prevalence of moderate-to-severe intellectual disability in the former group, advocating for an independent locus for psychomotor development neighboring MEIS2.

Published

2019

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

Author

Lumaka A, Race V, Peeters H, Corveleyn A, Coban-Akdemir Z, Jhangiani SN, Song X, Mubungu G, Posey J, Lupski JR, Vermeesch JR, Lukusa P, and Devriendt K

Subjects

Adolescent, Adult, Algorithms, Child, Child, Preschool, Comparative Genomic Hybridization, Democratic Republic of the Congo epidemiology, Developmental Disabilities epidemiology, Disease Management, Facies, Female, Genetic Markers, Genetic Testing, Homeodomain Proteins genetics, Humans, Infant, Intellectual Disability epidemiology, Male, Phenotype, Syndrome, Transcription Factors genetics, Trinucleotide Repeat Expansion, Trinucleotide Repeats, Exome Sequencing, Workflow, X Chromosome Inactivation, Young Adult, Developmental Disabilities diagnosis, Developmental Disabilities genetics, Genetic Association Studies, Genetic Predisposition to Disease, Intellectual Disability diagnosis, Intellectual Disability genetics

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., (© 2018 Wiley Periodicals, Inc.)

Published

2018

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

Author

Louw JJ, Corveleyn A, Jia Y, Hens G, Gewillig M, and Devriendt K

Subjects

Child, Preschool, Chromosome Deletion, Cleft Palate physiopathology, Exome genetics, Female, Heart physiopathology, Heart Septal Defects genetics, Heart Septal Defects physiopathology, Humans, Intellectual Disability physiopathology, Mutation, Sequence Analysis, DNA, Cleft Palate genetics, Heart growth & development, Homeodomain Proteins genetics, Intellectual Disability genetics, Transcription Factors genetics

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.)

Published

2015